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Assessing Cardiovascular Disease with Biomarkers

Posted in Biomarkers & Medical Diagnostics, CABG, Computational Biology/Systems and Bioinformatics, Frontiers in Cardiology and Cardiovascular Disorders, Origins of Cardiovascular Disease, PCI, Population Health Management, Nutrition and Phytochemistry, Proteomics, Systemic Inflammatory Response Related Disorders, tagged American College of Cardiology, BNP, Brain natriuretic peptide, Cardiovascular disease, Heart disease, Heart Failure, Journal of American College of Cardiology, Larry H. Bernstein, myocardial infarction, Risk factor on December 25, 2012| 22 Comments »

English: Amino acid sequence of the molecule of the brain natriuretic peptide (BNP) 32 (functional). Português: Sequência de aminoácidos da molécula de BNP 32 (funcional). (Photo credit: Wikipedia)

Assessing Cardiovascular Disease with Biomarker

Author and Curator: Larry H Bernstein, MD, FCAP

A Changing expectation from cardiac biomarkers.

This article on Assessing Cardiovascular Disease with Biomarkers will demonstrate the unique role in the discipline evolution that each of the following biomarkers has played in our understanding of CVD risk:

The article is introduced with an entire section on the evolution of our knowledge of cardiac biomarkers and how concepts from thermodynamics have transformed
the way we investigate biochemical mechanisms, and how we have gone from a macro- to a micro- landscape of high complexity. The same concepts from physics
have also transformed the mathematical stage upon which we model data. BIG Data is not just about business! We have entered a new domain of knowledge enabling.

(1) Enzymes and Isoenzymes

AST, ALT, LD, alkaline phosphatase
Isoenzymes evolution and genomic loci for polypeptides
Emergence of pathway divergence and regulation from gene-loci peptide changes
A reflection to implications for biomarkers and therapeutic development based on critical links

(2) Natriuretic Peptides

Cause of Death: silent cardiac target organ damage (cTOD) (no so sign of cardiac disease)
B Type natriuretic peptide in evolution of CHF
2D and Doppler echocardiography and BNP serum level
Amino terminal pro B-type Natriuretic Peptide
Renal Effect on NT-proBNP
pro-atrial natriuretic peptide

(3) CRP as Biomarker, theory that lowering the C-reactive protein (CRP) level with statin therapy is predictive of cardiovascular outcomes independent of lowering the low-density lipoprotein (LDL) cholesterol level

(4) CRP as an Inflammatory Agent

Acute phase reaction is a systemic response: physiological condition in the beginning of an inflammatory process.

(5) troponins and hs-troponins (I, T)

(6) New Candidate Biomarkers for NSTEMI

(7) Guidelines for Cardiovascular Risk Assessment

(8) Statistical Issues to be Resolved

Historical perspective

The use of cardiac markers emerged in the late 1950s, when the physician was faced with the problem of a patient with recent onset of squeezing, crushing, or heaviness in the chest, with or without a Q-wave or definitive ST elevation (acute injury), and perhaps a non specific elevation of the neutrophil count. A medical student at Albert Einstein Medical school at the time, Arthur Karmen identified the first enzymatic test for acute myocardial infarct (MI), serum glutamic oxaloacetic acid transaminase (SGOT), which is renamed Aspartate Aminotransferase (AST) in a seminal study with Wroblewski and LaDue[1]. The enzyme is ubiquitous, and the authors published another observation that the SGPT, now referred to as Alanine Aminotransferase, has a greater specific activity in liver and myocardial infarct can be distinguished from necrotizing liver disease by using AST and ALT. These two enzymes were among the three enzymes,with lactate dehydrogenase (LD) and alkaline phosphatase that appeared on the original Technicon (later Siemens) SMA-12 profile, prior to the designated panels used today. At that time it was common for the pathologist to stain the heart lesion at autopsy in identifying the “ischemic necrosis” postmortem.

In 1957 Hunter and Markert described the five isoenzymes of lactate dehydrogenase, the most anodal migrating pattern was associated with heart and the most cathodal isoenzymes with liver, the five bands being combinations of two subunits. These were described as different variants of the same enzyme having identical functions, but different tissue specific patterns, such that, enzyme variants have altered gene loci that results in an amino acid change but catalyze the same reaction. When mutation modifies the enzymatic catalysis, or its pattern of gene expression, then any of two (or more) variants may be favoured by natural selection and become specialized to different cell environments. His group suggested that a single gene might somehow encode an array of isozymes differing in “structural variations,” a concept that seems to presage our current understanding of alternative mRNA splicing and post-translational protein modification. A former student of George beadle, he transformed the “concept of one gene one enzyme” to “one gene one polypeptide”. By treating the enzyme with denaturing agents it was learned that LDH is a tetramer of two types of polypeptide chains (Appella and Markert, 1961). Thus the multiple-gene hypothesis was partially correct: Two different LDH subunits, each encoded by a distinct gene, re-sort themselves in various tetrameric combinations to give rise to five different isozymes (Markert, 1963). During the succeeding years Markert and his students and postdocs elucidated how the study of isozymes could contribute to our understanding of the biochemical variation that underlies cell differentiation and evolution, culminating in the new perspective presented in a Science paper (Markert et al., 1975) entitled “Evolution of a Gene.”

In the early 1960’s Nathan Kaplan postulated that the major LD-isoenzyme types were associated with fundamental differences in the metabolism of the tissue of origin, either catabolic (heart) or anabolic (liver), and skeletal muscle would appear to be in the same class as liver (ignore the ratio of fast and slow twitch), which was elaborated on further by studies of the flight wing patterns of birds. These isoenzymes not only had different migration in an electrophoretic field and could be separated chromatographically, but they also had different kinetic properties. They all have the same Km, but the purified heart LD is inhibited by a ternary complex of the enzyme, the NAD, and pyruvate that forms, slowing the reaction in the forward direction (pyruvate to lactate).

At about the same time, Masahiro Chiga discovered that adenylate kinase, the enzyme that converts ATP to ADP, from skeletal muscle can be inhibited by inorganic S (myokinase), which led Bernstein and Russell to publish on the identification of adenylate kinase from heart in myocardial infarction using sulfhydryl inhibition in J Molec Cellular Cardiology. Burton Sobel in the early 1970s showed that CK and the MB isoenzyme of CK, which has a more rapid increase and disappearance than the AST or LD , could be used to estimate the amount of cardiac damage in MI. This meant that a test could be done at any time of day or night with a result in less than an hour. He applied this to determining whether the extent of infarction was an important determinant of prognosis after myocardial infarction and furthermore, whether the extent of infarction could be modified by interventions that reduce myocardial oxygen requirements or increase myocardial oxygen supply. This work has had a major impact on how patients with acute myocardial infarction are treated and led to a reduction of mortality secondary to treatments, such as thrombolysis, that were validated initially with the methods developed. This led to an immunoassay for CK isoenzyme MB that was offered by Roche on the Cobas analyzer, and by Dupont on the ‘aca’. What emerged is a new imperative to reduce infarct size under the rubrick – “Time is Muscle”.

References

Karmen Arthur, Wróblewski Felix, LaDue John S. TRANSAMINASE ACTIVITY IN HUMAN BLOOD. J Clin Invest. 1955; 34(1):126–133.
LADUE JS, WROBLEWSKI F, KARMEN A. Serum glutamic oxaloacetic transaminase activity in human acute transmural myocardial infarction. Science 1956; 75(11).
Hunter, R. L. and C.L. Merkert. (1957) Histochemical demonstration of enzymes separated by zone electrophoresis in starch gels. Science 125: 1294-1295.
Bernstein L, Kerrigan M, Maisel H. Lactic dehydrogenase isoenzymes in lens and cornea. Exp Eye Res 1965; 5(3):999-1005. ICID: 844979
Nathan O. Kaplan Papers. MSS 0099. UC San Diego::Mandeville Special Collections Library.

Enzyme-coenzyme-substrate complex. of pyridine nucleotide depend. dehydrogenases 1958. box 39, folder 5.
Enzymatic studies with analogues of diphosphopyridine nucleotide 1959. box 39, folder 12.
Heterogeneity of the lactic dehydrogenases of new-born and adult rat heart as determined with enzyme analogs 1961. box 39, folder 37.
Regulatory effects of enzyme action 1961. box 39, folder 38.
Inhibition of dehydrogenase reactions by a substance formed from reduced dpn 1961. box 39, folder 40.
Lactic dehydrogenases: functions of the two types 1964. box 39, folder 67.
Lactate dehydrogenase – structure and function. 1964. box 40, folder 4.
Role of the two types of lactic dehydrogenases 1964. Box 40, folder 9.
Structural and functional properties of h and m subunits of lactic dehydrogenase 1965. Box 40, folder 12.

Bernstein LH, Everse J, Shioura N, Russell PJ. Detection of cardiac damage using a steady state assay for lactate dehydrogenase isoenzymes in serum. J Mol Cell Cardiol 1974; 6(4):297-315. ICID: 825597
Bernstein LH, Everse J. Determination of the isoenzyme levels of lactate dehydrogenase. Methods Enzymol 1975; 41 47-52.
Bernstein LH. Automated kinetic determination of lactate dehydrogenase isoenzymes in serum. Clin Chem 1977; 23(10):1928-1930. ICID: 825616
Bernstein LH, Scinto P. Two methods compared for measuring LD-1/total LD activity in serum. Clin Chem 1986; 32(5):792-796. ICID: 825581

Shell WE, Kjekshus JK, Sobel BE: Quantitative assessment of the extent of myocardial infarction in the conscious dog by means of analysis of serial changes in serum creatine phosphokinase activity. J Clin Invest 50:2614-2626, 1971.
Bergmann SR, Fox KAA, Ter-Pogossian MM, Sobel BE (Washington University), Collen D (University of Leuven): Clot-selective coronary thrombolysis with tissue-type plasminogen activator. Science 220:1181-1183, 1983.
Van de Werf F, Ludbrook PA, Bergmann SR, Tiefenbrunn AJ, Fox KAA, de Geest H, Verstraete M, Collen D, Sobel BE: Coronary thrombolysis with tissue-type plasminogen activator in patients with evolving myocardial infarction. N Engl J Med 310:609-613, 1984.

Adan J, Bernstein LH, Babb J. Can peak CK-MB segregate patients with acute myocardial infarction into different outcome classes? Clin Chem 1985; 31(2):996-997. ICID: 844986
Bernstein LH, Reynoso G. Creatine kinase B-subunit activity in serum in cases of suspected myocardial infarction: a prediction model based on the slope of MB increase and percentage CK-MB activity. Clin Chem 1983; 29(3):590-592. ICID: 825549
Bernstein LH, Horenstein JM, Sybers HB, Russell PJ. Adenylate kinase in human tissue. II. Serum adenylate kinase and myocardial infarction. J Mol Cell Cardiol 1973; 5(1):71-85. ICID: 825590

A Metabolic Functional Meaning of Existence of Isoenzymes

There are many examples of isozymes, such as glucokinase, a variant of hexokinase which is not inhibited by glucose 6-phosphate. It has different regulatory features and lower affinity for glucose (compared to other hexokinases). Alkaline and acid phosphatase isoenzymes were used briefly for a time in clinical diagnostics. These isoenzymes are oligomeric proteins that have distinct subunits that affect their binding with substrate. A distinctive type of protein that can form two or more different homo-oligomers, comes apart and changes shape to convert between forms is called a morpheein. The alternate shape may reassemble to a different oligomer, and the shape of the subunit dictates which oligomer is formed. Morpheeins can interconvert between forms under physiological conditions and can exist as an equilibrium of different oligomers. Features of morpheeins can be exploited for drug discovery. A small molecule compound can shift the equilibrium either by blocking or favoring formation of one of the oligomers. The equilibrium can be shifted using a small molecule that has a preferential binding affinity for only one of the alternate morpheein forms. This introduces the concept of allostericity. Most allosteric effects can be explained by a model put forth by Monod, Wyman, and Changeux, and also by a model described by Koshland, Nemethy, and Filmer. Both postulate that enzyme subunits exist in one of two conformations, tensed (T) or relaxed (R), and that relaxed subunits bind substrate more readily than those in the tense state. This concept provides a foundation for another generation of biomarkers than was the focus of the 20th century, and only has been investigated since the 1980’s, and takes another dimension after the completion of the Human Genome Project, opening a “Pandora’s box”. This moved biomedical science forward into an emerging field of ‘OMICs’, which tied small molecules into regulatory processes, transcription, and the possibility of identifying new biomarkers and developing new biomolecules that could modify disease progression.

References

Bu Z, Callaway DJ. “Proteins MOVE! Protein dynamics and long-range allostery in cell signaling”. Adv in Protein Chemistry and Structural Biology 2011; 83: 163–221. doi:10.1016/B978-0-12-381262-9.00005-7. PMID 21570668.
Monod J, Wyman J, Changeux JP. On the nature of allosteric transitions:A plausible model. J Mol Biol, May 1965; 12:88-118.
Koshland DE, Némethy G, Filmer D. Comparison of experimental binding data and theoretical models in proteins containing subunits. Biochemistry. Jan 1966; 5(1):365-8
Jaffe EK. “Morpheeins – a new structural paradigm for allosteric regulation”. Trends Biochem Sci 2005; 30(9): 490–497. doi:10.1016/j.tibs.2005.07.003. PMID 16023348.
Huang Z, Zhu L, Cao Y, Wu G, Liu X, et al. ASD: a comprehensive database of allosteric proteins and modulators. Nucleic Acids Res 2011; 39: D663-669

Fundamental Transformative Concepts Carried Over from Physics to Biomolecular Processes.

A colleague once noted that we are learning more and more about less and less. This is the remarkable evolution of our thinking from macrostates to microstates and segmentation of processes, further leading us to exploration of interactions between states. This has required a breakdown and a repeated remodeling or resynthesis of ideas based on new findings in science. It has gradually driven medicial science to a greater dependence on chemistry and physics in underlying principle. We can better envision the mechanism of evolution from the concepts put forth.

In 1824 Sadi Carnot published the concept that heat is lost in the conversion into work, using the term “caloric”, equivalent to entropy in the second law of thermodynamics. Clausius then develops the concepts of interior work in 1854, i.e. that “which the atoms of the body exert upon each other”, and exterior work, i.e. that “which arise from foreign influences [to] which the body may be exposed”, anticipating the concept of entropy. He enunciated the passage of the quantity of heat Q from the temperature T1 to the temperature T2 has the equivalence-value entropy, symbolized by S : dS = Q (1/T₂ – 1/T₁), which led to his 1865 statement on irreversible heat loss: I propose to name the quantity S the entropy of the system, after the Greek word [τροπη trope], the transformation. I have deliberately chosen the word entropy to be as similar as possible to the word energy.” In 1876, physicist J. Willard Gibbs, building on the work of Clausius, Hermann von Helmholtz and others, proposed that the measurement of “available energy” ΔG in a thermodynamic system could be mathematically accounted for by subtracting the “energy loss” TΔS from total energy change of the system ΔH, and in 1877, Ludwig Boltzmann formulated the alternative definition of entropy S defined as:

S = k_BlnΩ

where

kB is Boltzmann’s constant and

Ω is the number of microstates consistent with the given macrostate.

An analog to thermodynamic entropy is information entropy. Claude Shannon set out to mathematically quantify the statistical nature of “lost information” in phone-line signals and developed a concept of information entropy, a fundamental cornerstone of information theory. The close similarity between his new quantity and earlier work in thermodynamics is attributed to a visit and discussion with Jon von Neumann in 1949. Shannon then called the “measure of uncertainty” or attenuation in phone-line signals with reference to his new information theory. This led to the elucidation of a signal (as opposed to noise, by Solomon Kullback, which became the basis for the measure of an optimum diagnostic decision point of a laboratory test by Bernstein and Rudolph, related to Eugene Rypka’s “Syndromic Clustering”. The loop was closed by the Japanese mathematician Akaike, who brought Fisher’s statistical formulations and Kullback-Liebler distance into alignment. This is not a digression because it has been central to underlying principles in resolution in spectroscopy, and to classification of biochemical molecular features.

Although Boltzmann first linked entropy and probability in 1877, it seems the relation was never expressed with a specific constant until Max Planck first introduced k, and gave an accurate value for it (1.346×10−23 J/K, about 2.5% lower than today’s figure), in his derivation of the law of black body radiation in 1900–1901. Before 1900, equations involving Boltzmann factors were not written using the energies per molecule and the Boltzmann constant, but rather using a form of the gas constant R, and macroscopic energies for macroscopic quantities of the substance. The iconic terse form of the equation S = k log W on Boltzmann’s tombstone is in fact due to Planck, not Boltzmann. Planck actually introduced it in the same work as his h. Planck noted in his 1920 Nobel Prize acceptance : “:This constant is often referred to as Boltzmann’s constant, although, to my knowledge, Boltzmann himself never introduced it — a peculiar state of affairs.” The Kullback–Leibler divergence (also information divergence, information gain, relative entropy, or KLIC) is a non-symmetric measure of the difference between two probability distributions P and Q, was introduced by Solomon Kullback and Richard Leibler in 1951. KL-divergence of a model from reality may be estimated, to within a constant additive term, by a function (like the squares summed) of the deviations observed between data and the model’s predictions. When trying to fit parametrized models to data there are various estimators which attempt to minimize Kullback–Leibler divergence, such as, the familiar maximum likelihood estimator.

References

Planck, Max (2 June 1920), The Genesis and Present State of Development of the Quantum Theory (Nobel Lecture)
Kalinin M, Kononogov S. “Boltzmann’s Constant, the Energy Meaning of Temperature, and Thermodynamic Irreversibility”, Measurement Techniques 2005; 48 (7): 632–36, doi:10.1007/s11018-005-0195-9
Kullback S, Leibler RA “On Information and Sufficiency”. Annals of Mathematical Statistics 1951; 22 (1): 79–86. doi:10.1214/aoms/1177729694. MR 39968.
Kullback S (1959) Information theory and statistics (John Wiley and Sons, NY).
Jaynes ET(1957) Information theory and statistical mechanics, Physical Review 106:620
Jaynes ET(1957) Information theory and statistical mechanics II, Physical Review 108:171
Burnham KP and Anderson DR. (2002) Model Selection and Multimodel Inference: A Practical Information-Theoretic Approach, Second Edition (Springer Science, New York) ISBN 978-0-387-95364-9.
Rudolph RA, Bernstein LH, Babb J. Information induction for predicting acute myocardial infarction. Clin Chem 1988; 34(10):2031-2038. ICID: 825568

A New Imperative

Cardiovascular Biomarkers

I. BNP:

[A] Aids in the Prevention of Cardiac Events by Detecting Silent Ischemic Lesions and Selecting Patients for Imaging

12/17/12 · Emily Humphreys

Physicians use risk factors, such as history, exercise level, diabetes, blood pressure, lipid profiles, and other laboratory measurements to ascertain risk for cardiac events, which are not foolproof in predicting all cardiac events. Nonetheless, 40% to 50% of sudden cardiac deaths (SCD) occur before risk factors are able to predict cardiac events.^2,3 Those who die suddenly with no so sign of cardiac disease often have silent cardiac target organ damage (cTOD). While patients with silent ischemia have a 21-fold increase in risk of a coronary event.⁴ It has also been shown that cTODs such as left ventricular hypertrophy (LVH), left ventricular systolic dysfunction (LVSD), left ventricular diastolic dysfunction (LVDD), and left atrial enlargement (LAE) each independently predict cardiovascular events. ^5,6,7,8 Nadir et al. hypothesized that identification of silent cTOD would aid in the prevention of cardiovascular events, including SCDs.⁹ To identify cTOD present, The Nadir group evaluated several known cardiac biomarkers including: B-type natriuretic peptide (BNP), high-sensitivity cardiac troponin T (hs-cTnT), microalbuminuria, the estimated glomerular filtration rate, and uric acid. The lab results of 300 asymptomatic individuals recruited for the study were compared with primary screening using transthoracic echocardiography, stress echocardiography, and/or myocardial perfusion imaging.

34% of study volunteers had evidence of a cTOD. Out of all biomarkers analyzed, BNP levels were significantly higher in those with cTOD compared with those without. BNP levels were also higher in those who had more than one form of cTOD compared with those who had a single form of cTOD.
Hs-cTnT also performed well, but BNP levels had the highest correlation to imaging data. The gold standard diagnostic tool for cardiovascular disease is imaging studies, such as echocardiography.
It is not standard practice to investigate healthy individuals for possible cTOD and would be costly and time consuming to perform imaging on these individuals.
Biomarkers like BNP could be used as a primary screening tool with follow-up image studies performed, if necessary.

The eventual hope is to reduce the mortality of cardiovascular diseases and prevent silent cTOD from leading to more serious and potentially life-threatening cardiac events.

References

1. Roger, V.L. (2012) ‘AHA statistical update: Heart disease and stroke statistics-2012 update. A report from the american heart association‘, Circulation, 125 (2012), (pp. e2-e220)

2. Chiuve, S.E., et al., (2006) ‘Healthy lifestyle factors in the primary prevention of coronary heart disease among men: Benefits among users and nonusers of lipid-lowering and antihypertensive medications‘ Circulation, 114 (2006), (pp. 160-167)

3.De Vreede-Swagemakers, J.J., et al. (1997) ‘Out-of-hospital cardiac arrest in the 1990s: A population-based study in the Maastricht area on incidence, characteristics and survival‘, Journal of the American College of Cardiology, 30 (1997), (pp. 1500-1505)

4. Rutter, M.K., et al. (2002) ‘Significance of silent ischemia and microalbuminuria in predicting coronary events in asymptomatic patients with type 2 diabetes‘, Journal of the American College of Cardiology, 40 (2002), (pp. 56-61)

5. Tsang, T.S., et al. (2003) ‘Prediction of risk for first age-related cardiovascular events in an elderly population: The incremental value of echocardiography‘, Journal of the American College of Cardiology, 42 (2003), (pp. 1199-1205)

6. Gosse, P., (2005) ‘Left ventricular hypertrophy—the problem and possible solutions‘,The Journal of International Medical Research, 33 (Suppl 1) (2005), (pp. 3A-11A)

7. Benjamin, E.J., et al. (1995) ‘Left atrial size and the risk of stroke and death‘ The Framingham Heart Study Circulation, 92 (4), (pp. 835-41)

8. Redfield, M.M., et al. (2003) ‘Burden of systolic and diastolic ventricular dysfunction in the community: Appreciating the scope of the heart failure epidemic‘, JAMA, 289 (2003), (pp. 194-202)

9. Nadir, M.A., et al., (2012) ‘Improving the primary prevention of cardiovascular events by using biomarkers to identify individuals with silent heart disease‘, Journal of American College of Cardiology, 60 (11), (pp. 960-968) Tags: cardiovascular biomarker, cardiovascular disease, cardiovascular risk factors, cTOD

[B] Evaluating CHF patients in the emergency department

The role of B-type natriuretic peptide in the evaluation of congestive heart failure patients in emergency department

Congestive heart failure (CHF) is a severe cardiovascular disorder seen in the Emergency Department (ED). B-type Natriuretic Peptide (BNP) is usually ordered to evaluate the CHF severity.

However, it is difficult to interpret serum BNP level when different clinical entities existed.

The aim of this study is to illustrate the correlation between serum BNP level and

relevant clinical variables and
further determine the role of serum BNP in different CHF patients.

High variability of serum BNP levels exists in CHF patients with weak-to-moderate correlation effects particularly on obesity and diastolic/systolic HF.

Physicians should be cautious on interpreting BNP in different CHF populations.

Open Journal of Clinical Diagnostics scirp.org

[C] NT-proBNP compared with ECHO

Comparison of N-Terminal Pro B-Natriuretic Peptide and Echocardiographic Indices in Patients with Mitral Regurgitation. Shokoufeh Hajsadeghi1, Niloufar Samiei2, Masoud Moradi3, Maleki Majid2, et al. Corresponding author email: masoud_moradi65@yahoo.com

Abstract

Introduction: Echocardiographic indices can form the basis of the diagnosis of systolic and diastolic left ventricular (LV) dysfunction in patients with Mitral regurgitation (MR). However, using echocardiography alone may bring us to a diagnostic dead-end. The aim of this study was to compare N-Terminal pro B-natriuretic peptide (BNP) and echocardiographic indices in patients with mitral regurgitation.

Methods: 2D and Doppler echocardiography and BNP serum level were obtained from 54 patients with organic mild, moderate and severe MR.

Results: BNP levels were increased with symptoms in patients with mitral regurgitation (NYHAI: 5.7 ± 1.1, NYHAII: 6.9 ± 1.5, NYHAIII: 8.3 ± 2 pg/ml, P , 0.001). BNP plasma level were significantly correlated with MPI (myocardial performance index)(r = 0.399, P = 0.004), and following echocardiographic indices: LVEDV (r = 0.45, P , 0.001), LVESV (r = 0.54, P , 0.001), LVEDD (r = 0.48, P , 0.001), LVESD (r = 0.54, P , 0.001), dp/dt (r = −0.32, P = 0.019) and SPAP (r = 0.4, P = 0.006).

Conclusion: The present study showed that BNP may be useful in patients with MR and may confirm echocardiographic indices.

Keywords: mitral regurgitation, N-Terminal pro-B natriuretic peptide, echocardiographic indices.

The hypothesis assumes that there is a linear sequence of most effective screening that comes out of this study, from a b-type natriuretic peptide to the imaging. It’s not clear that that is the case, and moreover, silent myocardial infarct is taken and lumped with other serious conditions affecting the myocardium, presumably through compromise of the end-artery circulation to the heart (R, L, and circumflex coronaries). There is no mention of whether the patients were screened out for peripheral, carotid, or other associated artery disease (superior mesenteric).

I’ll assume that that is the case. I see a problem with a linear, monothetic, “gold standard” approach, when the disease and the diagnosis of it is multivariate and requires a method that uses a classificatory approach. We’ll return to that.

English: A Wiggers diagram, showing the cardiac cycle events occuring in the left ventricle. (Photo credit: Wikipedia)

[D] reference normal for NT-proBNP

ABSTRACT

Background: The natriuretic peptides, B-type natriuretic peptide (BNP) and NT-proBNP that have emerged as tools for diagnosing congestive heart failure (CHF) are affected by age and renal insufficiency (RI).This study evaluates the reference value for interpreting NT-proBNP concentrations. Increasing concentrations of NT-proBNP are associated with co-morbidities, not merely CHF, resulting in altered volume status or myocardial filling pressures.

Methods: NT-proBNP was measured in a population with normal trans-thoracic echocardiograms (TTE) and free of anemia or renal impairment.

Selection of Patients: Study participants were seen in acute care for symptoms of shortness of breath suspicious for CHF.

Results: The median NT-proBNP for patients under 50 years is 27.6 pg/ml with an upper limit of 445 pg/ml, and for patients over 50 years the median was 142.3 pg/ml with an upper limit of 475.3 pg/ml. We introduce a transformed NT-proBNP that normalizes for decrease in glomerular filtration rate and eliminates the age factor.

Conclusion: We suggest that NT-proBNP levels can be more accurately interpreted only after removal of the major co-morbidities that affect an increase in this peptide in serum. The PRIDE study guidelines should be applied until presence or absence of comorbidities is diagnosed. With no comorbidities, the reference range for normal over 50 years of age can be reduced below 800 pg/ml. The effect shown in previous papers likely is due to increasing concurrent comorbidity with age.

Key Words: Congestive Heart Failure, Natriuretic peptides, Anemia, Chronic renal insufficiency

Statistical treatment:

The combined acute and blood donor study sets were kept separate and each analyzed for central tendency, distribution and variability. The two were combined after the comorbidities described above were extracted from the acute care study group. This resulted in a population that should be representative of an unaffected study population that could be used to establish a most representative reference range. The database was replicated several times and then patient rows were randomly deleted until there was an expanded combined and mixed data set with 6,700 entries. All of the database sets were used for analyses.

The results are reported in means with p < 0.05 as the measure of significance for difference between means. Independent Student’s t-tests were applied comparing NT-proBNP and anemia. Univariate ANOVAs were used to compare NT-proBNP levels with varying ranges of hemoglobin and age using SPSS 15.0 (SPSS, Chicago, IL). A linear regression analysis with linear fitting and confidence interval was performed using SYSTAT 12 (SYSTAT, San Jose, CA). The results are reported in means with p < 0.05 as the measure of significance for difference between means. Linear regression analysis, Independent Student’s t and Mann-Whitney tests were applied comparing NT-proBNP for age intervals. Reference range was determined using MedCalc 9.2.0.0 (Mariakerke, Belgium).

We observe the following changes with respect to NT-proBNP and age:

Sharp increase in NT-proBNP at over age 50
Increase in NT-proBNP at 7 percent per decade over 50
Decrease in eGFR at 4 percent per decade over 50
Slope of NT-proBNP increase with age is related to proportion of patients with eGFR less than 90
NT-proBNP increase can be delayed or accelerated based on disease comorbidities

Adjustment of the NT-proBNP for eGFR and for age over 50 difference

We have carried out a normalization to adjust for both eGFR and for age over 50:

Take Log of NT-proBNP and multiply by 1000
Divide the result by eGFR (using MDRD[9] or Cockroft Gault[10])
Compare results for age under 50, 50-70, and over 70 years
Adjust to age under 50 years by multiplying by 0.66 and 0.56.

GFR (mL/min/1.73 m2) = 186 x (Scr)-1.154 x (Age)-0.203 x (0.742 if female) x (1.210 if African-American) (conventional units)

The equation does not require weight because the results are reported normalized to 1.73 m2 body surface area, which is an accepted average adult surface area.

Comparison of the mean + standard deviation of 607 blood donors and NYMH inpatients for the MDRD and Cockroft Gault (eCG), respectively gave 114.3, 43.7(MDRD); 105.0, 40.1 (eCG). The eCG is predicted by the regression: eCG = 0.059 + 0.918*MDRD. The mean + standard deviation for the age under 50 years and 50 or older is 106.5 + 14.7, 100.9 + 14.5 (MDRD); and 102.5 + 18.5, 98.4 + 20.8 (eCG). These differences are significant at < 0.0001, and 0.010, respectively.

The means comparison of the normalized NT-proBNP (NKLog[NT-proBNP]/eGFR) results in 23.4 and 18.7 for 307 non-donors and 300 donors, significant at p < 0.0001, assuming unequal variance). The difference is not significant for the MDRD normalized NT-proBNP (16.5, 6.6). The normalized by eCG result for 324 under age under 50 years and 283 age 50 years and older is 17.7 versus 18.2, significant at p = 0.0001. The MDRD calculated adjustment is 16.8 vs 16.9, which is not significant. The relationship between these is NKLog(NT-proBNP)/eCG = 4.47 + 0.948*NKLog(NT-proBNP)/MDRD. Figure 4 is a plot of the regression of NKLog(NTproBNP)/MDRD vs NKLog(NTproBNP)/eCG predicted over the full study population.

The reference range for the normalized Klog(NT-proBNP)/MDRD is described by a mean 13.99, median 13.12, and standard deviation 6.14 with a nonparametric upper limit of 24.7. A ROC curve is constructed comparing the NT-proBNP, the NKLog(NTproBNP)/MDRD and the ratio NTproBNP to NKLog(NTproBNP)/MDRD in the expanded full database. The area under the curve is 0.944 (0.938-0.950) for NKLog(NTproBNP)/MDRD with a base of 571 patients with early CHF and 6115 patients without. The reference range for NKLog(proBNP)/MDRD can be referenced to the percentiles as follows: 20, 8.78; 40, 11.92; 60, 14.85; 90, 21.10; 95, 24.73; 97.5, 29.54.

Conclusion: We suggest that NT-proBNP levels can be accurately assessed only after removal of the major confounding co-morbidities that increase this peptide in serum. We established our new range after establishing absence of co-morbidities. The value of this approach for screening purposes is an allowance for a considerably lower reference normal with a higher specificity based on the donor studies and the mixture model. This study finds that the reference range for NT-proBNP is age-dependent past age 50 years, mainly as the change relates to eGFR, and we introduce an age adjusted alternative measure, the normalized NT-proBNP using the MDRD transformation described.

NT-pro BNP reference range with blood donors and patients

Measure NT-proBNP (pg/ml) After trimming extremes

Highest 1110 599.4

Arithmetic mean 179.6 118.2

Geometric mean 68.7 54.4

Median 52.6 42.6

Standard deviation 250.5 150.6

D’Agostino-Pearson P = 0.0026 P = 0.0091

97.5%

< 50 years 526.9 445.0

> 50 years 1000 565.0

Upper Limit of Normal 772.9 475.3

95% confidence interval 637.1 – 873.73 442.7 – 531.0

Bernstein LH, Zions MY, Alam ME, Haq SA, Heitner JF, et al. What is the best approximation of reference normal for NT-proBNP? Clinical Levels for Enhanced Assessment of NT-proBNP (CLEAN)

Renal Effect on NT-proBNP

NT-proBNP is excreted by the kidney. Therefore, GFR has to be taken into account in adjusting the reference range. BNP, unlike the propeptide, is eliminated 80% by vascular endothelium. What would be the effect of vascular endothelium erosion? We don’t know.

The Cockroft Gault equation is widely used in hospitals for adjusting medication doses in hospital patients. The MDRD equation was developed for patients with renal insufficiency and has been shown to be comparable to CG for the population the MDRD is applied. However, the MDRD is only reported to a CLCR of only 60 ml/min and is not validated for age over 65 years. On the other hand, the body weight and BMI, necessary for calculating the CG formula are not routinely done for all patients or in all hospitals. We used 307 inpatients and calculated the MDRD up to 100 ml/min/m2, then used the results to predict the CG. The regression for MDRD versus the CG resulted in an r = 0.884, and a regression equation: CG = -21.1 + 1.172*(MDRD). The initial prediction of CG from MDRDe from 198 of the patients is defined by the regression: CGe = -64.6 + 1.866*MDRDe. (Deming)(95% CI: Intercept -84.5 to -42.8; slope 1.40 to 2.33). The means, medians, standard deviations, and 97.5^th percentiles, respectively, of the age, MDRDe and CGe (calculated from weight data) for the 307 patients are: age- 61.2, 62.0, 17.4, 91.3; MDRD – 121.5, 107.5, 55.9, 212.3; CG – 111.7, 98.7, 51.4, 195.0.

The NT-proBNP was adjusted using a log transform and the estimated GFR (glomerular filtration rate by the original method of Levey et al. The result for reference corrected Nt proBNP is shown in Table 2.

Table 2.

Kruskal-Wallis test

Data	KLOGNTPR
Factor codes	MDRD60

Sample size

440

Factor	n	Average Rank
0	344	174.11
1	96	386.73

Test statistic	209.8311
Corrected for ties Ht	209.8313
Degrees of Freedom (DF)	1
Significance level	P < 0.0001

[E] Mid-region proANP in Emergency Room

Mid-region pro-hormone markers for diagnosis and prognosis in acute dyspnea: results from the BACH (Biomarkers in Acute Heart Failure) trial.

J Am Coll Cardiol 2010 May 11;55(19):2062-76 (ISSN: 1558-3597)

Maisel A; Mueller C; Nowak R; Peacock WF; Landsberg JW; Ponikowski P; Mockel M; Hogan C; Wu AH; Richards M; Clopton P; Filippatos GS; Di Somma S; Anand I; Ng L; Daniels LB; Neath SX; Christenson R; Potocki M; McCord J; Terracciano G; Kremastinos D; Hartmann O; von Haehling S; Bergmann A; Morgenthaler NG; Anker SD
VA San Diego Healthcare System, San Diego, California 92161, USA. amaisel@ucsd.edu.

OBJECTIVES: Our purpose was to assess the diagnostic utility of mid–regional pro-atrial natriuretic peptide (MR-proANP) for the diagnosis of acute heart failure (AHF) and the prognostic value of mid–regional pro-adrenomedullin (MR-proADM) in patients with AHF. BACKGROUND: There are some caveats and limitations to natriuretic peptide testing in the acute dyspneic patient. METHODS: The BACH (Biomarkers in Acute Heart Failure) trial was a prospective, 15-center, international study of 1,641 patients presenting to the emergency department with dyspnea. A noninferiority test of MR-proANP versus B-type natriuretic peptide (BNP) for diagnosis of AHF and a superiority test of MR-proADM versus BNP for 90-day survival were conducted. Other end points were exploratory. RESULTS: MR-proANP (> or =120 pmol/l) proved noninferior to BNP (> or =100 pg/ml) for the diagnosis of AHF (accuracy difference 0.9%). In tests of secondary diagnostic objectives, MR-proANP levels added to the utility of BNP levels in patients with intermediate BNP values and with obesity but not in renal insufficiency, the elderly, or patients with edema. Using cut-off values from receiver-operating characteristic analysis, the accuracy to predict 90-day survival of heart failure patients was 73% (95% confidence interval: 70% to 77%) for MR-proADM and 62% (95% confidence interval: 58% to 66%) for BNP (difference p < 0.001). In adjusted multivariable Cox regression, MR-proADM, but not BNP, carried independent prognostic value (p < 0.001). Results were consistent using NT-proBNP instead of BNP (p < 0.001). None of the biomarkers was able to predict rehospitalization or visits to the emergency department with clinical relevance. CONCLUSIONS: MR-proANP is as useful as BNP for AHF diagnosis in dyspneic patients and may provide additional clinical utility when BNP is difficult to interpret. MR-proADM identifies patients with high 90-day mortality risk and adds prognostic value to BNP. (Biomarkers in Acute Heart Failure [BACH]; NCT00537628). [Copyright 2010 American College of Cardiology Foundation. Published by Elsevier Inc. All rights reserved.].

Comment In: RefSource:J Am Coll Cardiol. 2010 May 11; 55(19):2077-9/PMID:20447529

II. CRP

[A] Predictor of benefit of lowering CRP with statin

Sever PS, Poulter NR, Chang CL, et al; ASCOT Investigators. Evaluation of C-reactive protein prior to and on-treatment as a predictor of benefit from atorvastatin: observations from the Anglo-Scandinavian Cardiac Outcomes Trial. Eur Heart J. 2012;33:486-494

The theory that lowering the C-reactive protein (CRP) level with statin therapy is predictive of cardiovascular outcomes independent of lowering the low-density lipoprotein (LDL) cholesterol level was first advanced by the JUPITER investigators.^[1]

This study further fueled the debate on whether CRP measurement should be routine for monitoring cardiovascular disease risk. The ASCOT investigators entered this debate when they analyzed data from their trial to determine whether on-statin C-reactive protein level was associated with cardiovascular outcomes.^[4]
The data in the nested case-control study were from persons recruited to ASCOT in the United Kingdom and Ireland, 9098 of whom were randomly assigned in the blood pressure-lowering arm to receive either amlodipine with or without perindopril or atenolol with or without bendroflumethiazide.^[5] Within the whole blood-pressure-lowering group, 4853 persons with a total cholesterol level of 6.5 mmol/L or less (≤ 250 mg/dL) were further randomized to receive atorvastatin or placebo as part of the lipid-lowering arm.^[6]
For the case-control study, 485 cardiovascular cases were age- and sex-matched with 1367 controls. As expected, the investigators found that baseline LDL cholesterol and CRP levels both predicted cardiovascular events.
However, neither the baseline nor the on-treatment CRP level was related to the magnitude of statin efficacy in the prevention of cardiovascular events, whereas the on-treatment LDL cholesterol level was strongly predictive. Including CRP in the Framingham model resulted in a “modest” (2.1%) improvement in risk prediction overall.

The investigators noted that this finding was in line with other prospective studies that showed statistically significant, but modest, absolute improvements with the use of CRP in clinical risk prediction.^[7,8] They concluded that “in this hypertensive population selected on the basis of traditional, common coexisting risk factors, CRP did not usefully improve the prediction of cardiovascular events and, critically, reduction in CRP associated with statin therapy was not a predictor of cardiovascular outcome alone or in combination with LDL-cholesterol.”

Eugene Braunwald downplayed the ASCOT investigators’ conclusions in observing “the ASCOT results, albeit quite limited in size, are in fact remarkably similar to those of the [CARE, AFCAPS/TexCAPS, REVERSAL, A to Z], and JUPITER trials, especially in light of the fact that the dose of atorvastatin [in ASCOT] was only 10 mg, while some of the other trials used considerably larger equivalent doses of statins.”

My own take on this is that for at least two decades, there was a belief that the LDL lowering was the main effect of statins, until the (deep frozen) specimens were reexamined from the Framingham study using a hs CRP assay. The investigation was to determine whether there is a predictor of CVD that is present when the traditional features are not present (which would have to include diabetes and hypertension). The basis for the use of hsCRP became to identify patients who had sufficient risk to be treated with a statin. The essential focus seemed to turn on whether statin treatment has efficacy in view of the differential between the LDL or the CRP on the magnitude of the effect. The muscular effect of a statin then comes into view with the size dose and length of treatment. However, the CRP measurement identified a relationship between development of the vascular disease and the inflammatory process independently of the STATIN treatment benefit.

Prof. Sever (Medscape): The key result that we found in the initial paper was that CRP, although an independent predictor of cardiovascular events in the hypertensive population, was really only a weak predictor, which is confirmed by the meta-analyses. Furthermore, when you incorporate CRP into a Framingham-style model, it really does not add any benefit or give any more information than if it had not been included in the model. LDL cholesterol is a much more important biomarker. Our second important conclusion addressed the question of whether, after starting a patient on statin therapy, the magnitude of lowering CRP by the statin and the level to which CRP has been reduced predicts cardiovascular outcome. The simple answer from our analyses was that it did not and that the benefits were all related to lowering LDL cholesterol. Our population comprised patients with stable hypertension and no history of coronary disease; likewise, the diabetes population in CARDS had no history of coronary heart disease. Oddly, PROVE IT-TIMI 22 involved persons who were selected from a high-risk coronary heart disease population simply because they had a high level of an inflammatory marker. So, to a certain extent, this is like comparing apples and oranges, and to find some unifying hypothesis on the basis of widely heterogeneous patient populations seems to be a little naive.

[B] Predictor of cardiovascular disease

Acute Phase Reactants as Novel Predictors of Cardiovascular Disease M. S. Ahmed, A. B. Jadhav, A. Hassan, and Qing H. Meng SRN Inflammation 2012; Article ID 953461, 18 pages. doi:10.5402/2012/953461

Acute phase reaction is a systemic response which usually follows a physiological condition that takes place in the beginning of an inflammatory process.
This physiological change usually lasts 1-2 days. However, the systemic acute phase response usually lasts longer.
The aim of this systemic response is to restore homeostasis.

These events are accompanied by upregulation of some proteins (positive acute phase reactants) and
downregulation of others (negative acute phase reactants) during inflammatory reactions.

Cardiovascular diseases are accompanied by the elevation of several positive acute phase reactants such as

C-reactive protein (CRP),
serum amyloid A (SAA),
fibrinogen,
white blood cell count,
secretory nonpancreatic phospholipase 2-II (sPLA2-II),
ferritin, and
ceruloplasmin.

Cardiovascular disease is also accompanied by the reduction of important transport proteins such as

albumin, transferrin,
transthyretin,
retinol-binding protein,
antithrombin, and
transcortin.

In this paper, we will be discussing the biological activity and diagnostic and prognostic values of acute phase reactants with cardiovascular importance.

The potential therapeutic targets of these reactants will be also discussed.

[C] CRP as an Inflammatory Biomarker

CRP is an acute phase protein [7, 8] produced in the liver in response to interleukin- (IL-) 6 which is stimulated, in turn, by tumour necrosis factor-α (TNF-α) and IL-1 [8, 9].

Recent studies suggest that CRP plays a pivotal role in many aspects of atherogenesis including

LDL uptake by macrophage,
release of proinflammatory cytokines,
expression of monocyte chemotactic protein-1,
intercellular adhesion molecule-1, and vascular cellular adhesion molecule-1 [10–12].

Activation of inflammation and the acute phase reaction appear to play an important role, not only in the pathogenesis of atherosclerosis, but also in the initiation of the acute coronary syndrome (ACS) [13,14]. Cesari et al. suggested that the inflammatory markers CRP, IL-6, and TNF-α are independent predictors of cardiovascular events in older persons [14].

Diagnostic Value

CRP is also an early ischemic marker and elevated CRP is predictive of future adverse events [22, 23]. High-sensitivity CRP (hs-CRP) rises acutely after tissue injury, including myocardial infarction (MI). Intense cytokine production and inflammatory cell infiltration occur in the area of ischemia and necrosis. This increase of hs-CRP levels, in part, correlates with infarct size [24, 25]

CRP can be also used for patients screening in the primary prevention population [36]. Ockene et al. indicated that CRP is generally expressed at low levels (<1 mg/L) in healthy adults and levels remain relatively stable in the absence of an acute inflammatory stimulus [37].

Patients with unstable angina and CRP >3 mg/L at discharge are more likely to be readmitted for recurrent cardiovascular instability or MI within 1 year [38].

Pietilä et al. indicated that hs-CRP measurement is the strongest correlative factor for future clinical events due to arterial inflammation, myocardial infarction, unstable angina, stroke, and peripheral vascular disease in both diseased and apparently healthy asymptomatic patients [40].

The CRP plasma level also is the best risk assessment in patients with

either stable or unstable angina,
long term after myocardial infarction, and
in patients undergoing revascularization therapies [41].

One study showed the only independent cardiovascular risk indicators using multivariate, age adjusted and traditional risk analysis were CRP and Total/HDL cholesterol ratio.
If CRP, IL-6, and ICAM-1 levels are added to lipid levels, risk assessment can be improved over lipids alone.
Moreover, serum CRP may indicate the vulnerability of the plaque [40].

Prognostic Value

elevation of hs-CRP levels predicts a poor cardiovascular prognosis [42].
The extent of the inflammatory response to injury appears to have prognostic significance, which is independent of the extent of myocardial injury.
hs-CRP response after MI has been shown to predict future CHD morbidity and mortality independent of infarct size [43].
CRP is also a predictor of incident type 2 diabetes. As well, it adds a prognostic information on vascular risk at all levels of the metabolic syndrome [44].

__________________________________________________________________________________________________________________________

III. Troponin(s) and hs-TnI/cTnT

Comparison of diagnostic accuracy between three different rules of interpreting high sensitivity troponin T results. Francesco Buccelletti; Leonarda Galiuto; Davide Marsiliani; Paolo Iacomini; et al. Intern Emerg Med 2012; 7, 365

Abstract

With the introduction of high sensitivity troponin-T (hs-TnT) assay, clinicians face more patients with ‘positive’ results but without myocardial infarction. Repeated hs-TnT determinations are warranted to improve specificity. The aim of this study was to compare diagnostic accuracy of three different interpretation rules for two hs-TnT results taken 6 h apart. After adjusting for clinical differences, hs-TnT results were recoded according to the three rules.

Rule1: hs-TnT >13 ng/L in at least one determination.
Rule2: change of >20 % between the two measures.
Rule3: change >50 % if baseline hs-TnT 14-53 ng/L and >20 % if baseline >54 ng/L.

The sensitivity, specificity and ROC curves were compared. The sensitivity analysis was used to generate post-test probability for any test result. Primary outcome was the evidence of coronary critical stenosis (CCS) on coronary angiography in patients with high-risk chest pain.

183 patients were analyzed (38.3 %) among all patients presenting with chest pain during the study period. CCS was found in 80 (43.7 %) cases.

The specificity was 0.62 (0.52-0.71), 0.76 (0.66-0.84) and 0.83 (0.74-0.89) for rules 1, 2 and 3, respectively (P < 0.01). Sensitivity decreased with increasing specificity (P < 0.01).

Overall diagnostic accuracy did not differ among the three rules (AUC curves difference P = 0.12). Sensitivity analysis showed a 25 % relative gain in predicting CCS using rule 3 compared to rule 1. Changes between two determinations of hs-TnT 6 h apart effectively improved specificity for CCS presence in high-risk chest pain patients.

There was a parallel loss in sensitivity that discouraged any use of such changes as a unique way to interpret the new hs-TnT results.

Advances in identifying NSTEMI biomarkers [Published 31 August 2012 | Article by Excerpta Medica | Tags: elderly, ami, biomarkers, diagnosis]

In the run-up to the ESC conference at the end of August, we review some recently published research on the hot topic of biomarkers for NSTEMI.

Prompt and accurate diagnosis of acute non-ST elevation myocardial infarction (NSTEMI) can be particularly challenging in elderly patients, as they often present with

atypical symptoms and/or have an inconclusive ECG.
the diagnostic value of cardiac troponin T (cTnT), an established marker of cardiac injury, is often limited as there is often non-coronary troponin elevation caused by concomitant conditions such as acute congestive heart failure.
Identifying new sensitive and specific biomarkers of NSTEMI in elderly patients is therefore important, and circulating microRNAs (miRs) are emerging as good candidates.

researchers evaluated the diagnostic potential of plasma levels of various miRs in elderly patients enrolled at presentation:

92 acute NSTEMI patients (complicated by congestive heart failure in three-quarters of cases),
81 patients with acute congestive heart failure without acute MI, and
99 age-matched healthy people (the control group).

The researchers, from centers in Italy, found that levels of miR-1, miR-21, miR-133a, and miR-423-5p were 3-10 times higher in the patients with NSTEMI, compared with controls. Levels of miR-499-5p, meanwhile, were more than 80 times higher in the NSTEMI patients compared with the patients in the control group.

Levels of miR-499-5p and miR-21 were also significantly higher in the NSTEMI group compared with the group of patients with acute congestive heart failure without acute MI.
The researchers also found that miR-499-5p was similar to cTnT in being able to distinguish NSTEMI patients from the other two groups.
Also, a subgroup analysis of patients with a modest elevation in cTnT level at presentation (0.03-0.10 ng/mL) revealed that miR-499-5p had a diagnostic accuracy superior both to cTnT and to high sensitivity cTnT in differentiating NSTEMI from acute congestive heart failure.

International Journal of Cardiology

________________________________________________________________________________________________________________________________________________________________________

IV. Predicting cardiovascular mortality in NSTEMI patients

[A] Japanese researchers studied 258 consecutive patients hospitalized for unstable angina and NSTEMI within 24 hours of the onset of chest symptoms, and followed them up for a median period of 49 months after admission. During this period there were 38 cardiovascular deaths (14.7%).

They reported that high-mobility group- box 1 (HMGB1), a nuclear protein and signaller of tissue damage, was “a potential and independent predictor of cardiovascular mortality in patients hospitalized for unstable angina and NSTEMI.

HMGB1,
cardiac troponin I,
Killip class greater than 1, and
age

were each independently and significantly associated with cardiovascular mortality.

……………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………

[B] William LaFramboise et al. BMC Med. 2012 Dec 5;10(1):157)
see Report by Aviva Lev-Ari (pharmaceuticalintelligence.com) Coronary artery disease in symptomatic patients referred for coronary angiography: Predicted by Serum Protein Profiles

Significant differences were detected in circulating proteins from patients requiring revascularization including increased apolipoprotein B100 (APO-B100), C-reactive protein (CRP), fibrinogen, vascular cell adhesion molecule 1 (VCAM-1), myeloperoxidase (MPO), resistin, osteopontin, interleukin (IL)-1beta, IL-6, IL-10 and N-terminal fragment protein precursor brain natriuretic peptide (NT-pBNP) and decreased apolipoprotein A1 (APO-A1). Biomarker classification signatures comprising up to 5 analytes were identified using a tunable scoring function trained against 239 samples and validated with 120 additional samples. A total of 14 overlapping signatures classified patients without significant coronary disease (38% to 59% specificity) while maintaining 95% sensitivity for patients requiring revascularization. Osteopontin (14 times) and resistin (10 times) were most frequently represented among these diagnostic signatures. The most efficacious protein signature in validation studies comprised osteopontin (OPN), resistin, matrix metalloproteinase 7 (MMP7) and interferon gamma (IFNgamma) as a four-marker panel while the addition of either CRP or adiponectin (ACRP-30) yielded comparable results in five protein signatures.

______________________________________________________________________________________________________________________________________________________

V. Assessing Cardiovascular Risk

Agency for Healthcare Research and Quality (AHRQ)

Assessing Cardiovascular Risk: Guideline Synthesis

Agency for Healthcare Research and Quality (AHRQ) Authors and Disclosures Posted: 03/01/2012

…………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………………..

The Third MI Definition: An Expert Interview With Joseph Alpert In the new definition, the diagnosis of acute MI remains unchanged: That is, it applies where there is evidence of myocardial necrosis in a clinical setting consistent with acute myocardial ischemia. However, the criteria for diagnosis have been updated, with an emphasis on the biomarker cardiac troponin.

The first essential criterion for diagnosis of MI is detection of a rise or fall in cardiac troponin, or CKMB if troponin is not available, with at least 1 value above the 99th percentile upper reference limit, plus at least 1 the following criteria:
Symptoms of ischemia;
ECG changes of new or presumed new ischemia (significant ST-segment T-wave changes or new left bundle branch block);
Development of pathologic Q waves on ECG; or
Imaging evidence of new loss of viable myocardium or new regional wall-motion abnormality.Other criteria include those for MI in sudden unexpected cardiac death and for MI during percutaneous coronary intervention (PCI) and coronary artery bypass graft surgery (CABG).

The guidance document supports the use of high-sensitivity cardiac troponin assays, especially for distinguishing myocardial injury not related to myocardial ischemia, such as that associated with heart failure or renal failure. These assays are available in Europe, and not in the United States. MI is designated as ST-segment elevation MI or non- ST-segment elevation MI, and as in the 2007 version, it is classified into 5 types on the basis of pathologic, clinical, and prognostic differences. These types have been updated in the latest version.

Type 1 MI (spontaneous MI) is related to atherosclerotic plaque rupture or other event leading to thrombus formation in ≥ 1 of the coronary arteries, leading to decreased myocardial blood flow with ensuing necrosis;
Type 2 MI arises from a condition other than CAD;
Type 3 MI is deemed to have occurred when cardiac death occurs with symptoms suggestive of myocardial ischemia, but without biomarker values having been obtained; and
Type 4 and 5 MIs are related to PCI and CABG, respectively, and have been redefined since 2007.

The new document also describes situations in which troponin levels are elevated in conditions where myocardial injury with necrosis is associated with predominantly nonischemic myocardial injury, such as heart failure, renal failure, myocarditis, arrhythmias, or pulmonary embolism.

__________________________________________________________________________________________________________________________________________________________________________

VI Statistical Problems

The normal or “bell shaped” curve is a plot of numerical values along the x-axis and the frequency of the occurrence on the y-axis. If the set of measurements occurs as a random and independent event, we refer to this as parametric, and the distribution of the values is a bell shaped curve with all but 2.5% of the values included within both ends, with the mean or arithmetic average at the center, and with 67% of the sample contained within 1 standard deviation of the mean. We view a reference range in terms of a homogeneous population. This means that while all values might not be the same, the values are scattered within a distance from the mean that becomes less frequent as the distance is larger so that we can describe a mean and a 95% confidence interval around the mean. In the problem we are discussing, the classic reference value could be determined with outliers removed, and it would most likely fit to a Receiver Operator Characteristic curve. This became blurred when the high sensitivity assay was introduced, which included NOISE, which is really not noise but heterogeneous elements related to [a] vascular events that are not caused by plaque rupture, or [b] ischemia related to “piecemeal necrosis” which continued might predict a serious future event. Hidden variables include – age, diurnal variation, racial factors, and disease (hypertension, CHF, type 2 diabetes, renal failure).

A majority have no ST elevation on EKG, considered definitive for AMI. This makes the finding of elevated and increasing cardiac specific enzyme or protein in serum of paramount importance for specifying damaged cardiac muscle in a context of insufficient circulation. We examine the classification of AMI using a combination of features of chest pain, EKG, and a sensitive cardiac marker, derived from the cardiac muscle filament. An optimum value for a test cutoff is, such as cTnT, can be derived without using a prior determination of disease status. This is an alternative to first carrying out a study with a training set, and then repeating it with a validation set, provided there is sufficient information for classifying the data.. We have to construct a self-classifying table of ordered classes that have assigned measurable risks. Haberman (4) discusses the underlying assumptions used by Magidson for association models of cross-classified data in calculating the maximum likelihood estimates (MLE) by using the log-likelihood ratio and a sum of squares representing deviations of parameters from their constraints. The Latent Class Analysis (LCA) developed by Magidson and Vermunt allows use of a traditional LCA or a regression model (Statistical Innovation. Belmont, MA). . The LCA model uses the variables – chest pain, EKG, and troponin T – to classify the data and to test the underlying structure using powerful fit measures, such as L². Chest pain has the value of “typical” or “other”. EKG has the value ST depression or any other (for a non Q-wave study). “cTnT” has the value assigned by rank in the scaling intervals. The results of such an analysis are displayed in Table 1.

Table 1. This LCA classification was constructed using the troponin T before hsTnT was available.

CTnT (mg/L)	MI (6%)	Not MI (94%)
0-0.03	0.0008	0.8485
0.031-0.055	0.0009	0.0791
0.056-0.080	0.0009	0.0369
0.081-0.099	0.0010	0.0106
0.10-0.199	0.2026	0.0238
> 0.20	0.7939	0.0012

Eugene Rypka. Syndromic classification: A process for amplifying information using S-Clustering. Nutrition 1996; 14(12: 827-829.

Stuart W Zarich, Keith Bradley, Inder Dip Mayall, Larry H Bernstein. Minor elevations in troponin T values enhance risk assessment in emergency department patients with suspected myocardial ischemia: analysis of novel troponin T cut-off values. Clin Chim Acta 2004; 343(1-2):223-229

Haberman SJ. Computation of maximum likelihood estimates in association models. J Am Stat Assoc 1995;90:1438-1446

Rudolph RA, Bernstein LH, Babb J. Information Induction for the Diagnosis of Myocardial Infarction. Clin Chem 1988; 34: 2031-8.

Vermoent JK, and Magidson J. Latent class cluster analysis. JA Hagenaars and AL McCutcheon (eds.), Advanced Latent Class Analysis. Cambridge, Cambridge University Press, 2000.

Bernstein LH, Qamar A, McPherson C, Zarich S. Evaluating a new graphical ordinal logit method (GOLDminer) in the diagnosis of myocardial infarction utilizing clinical features and laboratory data. Yale J Biol Med 1999; 72: 259-268.

__________________________________________________________________________________________________________________________________________________________________________

VII. Conclusions I have made a number of comments to follow up on. The diagnosis of myocardial infarct has been extended as a result of the emergence of the high sensitivity troponins, but the laboratory methods have not caught up with the technology as the identification of myocardial ischemia is broken down with fine granularity in order to

identify the high risk patients early
and manage them effectively at the earliest stage of disease evolution

We no longer ponder over

ECG findings of new Q-qave, not previously seen
ST elevation
T-wave inversion

These are an indication of plaque rupture. There are strong associations between CRP, hyperhomocysteinemia, and then add the troponins and b-type natriuretic and the pro b-type peptides. These associations have to be analyzed by “syndromic classification”, described by Eugene Rypka. The study first described found great value in the BNP and proBNP. Despite having the creatinine clearance, the NT-proBNP can’t be adequately interpreted without adjusting for the estimated glomerular filtration rate, and using a log transform for the high fold-increase with age.

There is much more to be done with capturing the information from the data we are generating. The problem of classification requires accurate data measurement, but it also requires that features in scaled data are combined in meaningful ways. That job is far from completed.

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Below I paste all discussions on this post that are taking place on LinkedIn Group: Innovations in Cardiology:

Kathy Dowd, AuD • I am an audiologist representing the Academy of Doctors of Audiology for an initiative of early identification of hearing loss in adults with chronic diseases, including cardiovascular disease, thyroid disease, diabetes, etc. I am working on a new product that will automatically screen hearing of patients with these conditions and route them to audiologists for evaluation, treatment and counseling. Hearing loss is unidentified for most adults for 7-10. The psychological impact of hearing loss includes depression, isolation, confusion and poor job performance. We are focused on educating healthcare professionals on the need to identify this ‘silent epidemic’ as a co morbidity with most major illnesses.

Aviva Lev-Ari, PhD, RN • Dr. William LaFramboise

Thank you for your comment above and the reference to your most recent publication. It is very helpful. We are on the same page on this topic.

May I bring to the attention of the readers three sources which are shading additional light on that matter.

To Stent or Not? A Critical Decision

To Stent or Not? A Critical Decision

Obstructive coronary artery disease diagnosed by RNA levels of 23 genes – CardioDx heart disease test wins Medicare coverage

http://pharmaceuticalintelligence.com/2012/08/14/obstructive-coronary-artery-disease-diagnosed-by-rna-levels-of-23-genes-cardiodx-heart-disease-test-wins-medicare-coverage/http://pharmaceuticalintelligence.com/?s=PCI

Follow William
William LaFramboise • Thank you Aviva. The CardioDx approach is promising with heavy commercial support for use in a primary care practitioner’s office. However, RNA acquisition, purification and qRT-PCR expression analysis takes 2-3 days, is performed off-site, derives from a small subset of circulating inflammatory cells and is not yet directly correlated with functional proteomics. So its value in the Emergency Room and Chest Clinic is currently limited. The proteomics test we published revealed systemic serum changes in a small number of proteins known to be involved in atherosclerosis. It has a faster turnaround time (minutes to hours) that could be implemented in an emergency room or chest clinic. We are predominantly interested in using our test to “rule out” symptomatic patients who currently undergo coronary angiography but do NOT have clinically significant CAD. Our goal is to eliminate unecessary catheterizations while catching all patients that should undergo coronary angiography with a high probability of percutaneous intervention. Currently, the patients we are targeting all undergo catheterization; our test will hopefully allow us to identify at least some of these patients who do not have CAD and eliminate this expensive and risky procedure. However, we are in the pioneering stages of developing our test so there are miles to go before we establish and validate clinical efficacy.

Larry

Larry Bernstein • What you have indicated is practical proteomics. There is more to be done in line with what Dr Lev-Ari has indicated based on additional voluminous literature. What you have done with a not so large data set, and probably underpowered looks very interesting.

I f you were willing to share the data, now that it is publihed, I think that we can sharpen the results using a method of “identifying anomalies”, and even come up with estimated probabilities for meaningful classes. I think that the best you can get is defined by Kullback-Liebler distance.

Larry H Bernstein, MD
larry.bernstein@gmail.com

Biomarker classification signatures comprising up to 5 analytes were identified using a tunable scoring function trained against 239 samples and validated with 120 additional samples. A total of 14 overlapping signatures classified patients without significant coronary disease (38% to 59% specificity) while maintaining 95% sensitivity for patients requiring revascularization. Osteopontin (14 times) and resistin (10 times) were most frequently represented among these diagnostic signatures. The most efficacious protein signature in validation studies comprised osteopontin (OPN), resistin, matrix metalloproteinase 7 (MMP7) and interferon gamma (IFNgamma) as a four-marker panel while the addition of either CRP or adiponectin (ACRP-30) yielded comparable results in five protein signatures.

Proteins in the serum of CAD patients predominantly reflected (1) a positive acute phase, inflammatory response and (2) alterations in lipid metabolism, transport, peroxidation and accumulation.

Follow William
William LaFramboise • Our study (http://www.ncbi.nlm.nih.gov/pubmed/23216991) comprised discovery research using targeted immunochemical screening of retrospective patient samples using both Luminex and Aushon platforms as opposed to shotgun proteomics. Hence the costs constrained sample numbers. Nevertheless, our ability to predict outcome substantially exceeded available methods:

DISCUSSION
The Framingham CHD scores were statistically different between groups (P <0.001, unpaired Student’s t test) but they classified only 16% of the subjects without significant CAD (10 of 63) at a 95% sensitivity for patients with CAD. In contrast, our algorithm incorporating serum values for OPN, RES, CRP, MMP7 and IFNγ identified 63% of the subjects without significant CAD (40 of 63) at 95% sensitivity for patients with CAD. Thus, our multiplex serum protein classifier correctly identified four times as many patients as the Framingham index.

The addition of clinical variables to our scoring system should improve the acuity of our test as we move into the next phase. I appreciate your input and will contact you directly for further insights

Larry Bernstein • Bill La Fram..

our algorithm incorporating serum values for OPN, RES, CRP, MMP7 and IFNγ identified 63% of the subjects without significant CAD (40 of 63) at 95% sensitivity for patients with CAD

I think you can improve the algorithm with strong clinical features. The Goldman algorithm is stronger than the Framingham Index. Maybe its because the FI is epidemiological and is a measure of long term risk being present and does not indicate significant features at the time of presenting. The best features of the Goldman algorithm (without lab work) are – ECG (which may be arguable with NSEMI), but the presence of Afib or tachyarrhythmia could be added to that in weighting, and radiation actually should include symptoms of gall bladder (vagal nerve branch), and onset, characteristic and duration of pain, and SOB.

In your algorithm there isn’t any assessment of the hypercoagulable state, blood flow or Viscosity. There is a strong relationship between hyperhomocysteinemia and CVD, and the HHCys has ties to impaired methyl group transfers that maybe proinflammatory through more than one interaction: countering eNOS, related to Lp(a), un unknown relationship to iNOS (which becomes a counterpoise to eNOS), an effect on blood flow and viscosity, and a relationship to platelet aggregation.

Lp(a) was originally considered of less weight, except that it occurred in thin people from Asian Indian descent. The relationship to apo(B) and to dense LDL particles is now a factor. Sam Filligane uses Lp(a) in his ambulatory practice, and he also uses the PLAC test that Aviva has posted on.

The biggest problem we have is the amount of variability in the data physicians use. It makes metaanalysis a poor solution to the problem. The standardization of laboratory “panels” set up after CLIA 88 puts a real burden on the physician for unsubstantiated “cost benefits” in the light of today’s knowledge.

English: Four chamber view on cardiovascular magnetic resonance imaging. (Photo credit: Wikipedia)

Other related articles on Assessing Cardiovascular Disease with Biomarkers published on this Open Access Online Scientific Journal, include the following:

Dr. Lev-Ari’s research on Assessing Cardiovascular Disease with Biomarkers includes

Biomarkers in vascular biology,
Biomarkers in molecular cardiology and
circulating Endothelial Progenitor Cells (cEPCs) as a Biomarker for cardiovascular marcovascular disease risk

Lev-Ari, A., (2012U). Cardiovascular Outcomes: Function of circulating Endothelial Progenitor Cells (cEPCs): Exploring Pharmaco-therapy targeted at Endogenous Augmentation of cEPCs

http://pharmaceuticalintelligence.com/2012/08/28/cardiovascular-outcomes-function-of-circulating-endothelial-progenitor-cells-cepcs-exploring-pharmaco-therapy-targeted-at-endogenous-augmentation-of-cepcs/

Lev-Ari, A., (2012T). Endothelial Dysfunction, Diminished Availability of cEPCs, Increasing CVD Risk for Macrovascular Disease – Therapeutic Potential of cEPCs

http://pharmaceuticalintelligence.com/2012/08/27/endothelial-dysfunction-diminished-availability-of-cepcs-increasing-cvd-risk-for-macrovascular-disease-therapeutic-potential-of-cepcs/

Lev-Ari, A., (2012S). Vascular Medicine and Biology: CLASSIFICATION OF FAST ACTING THERAPY FOR PATIENTS AT HIGH RISK FOR MACROVASCULAR EVENTS Macrovascular Disease – Therapeutic Potential of cEPCs

http://pharmaceuticalintelligence.com/2012/08/24/vascular-medicine-and-biology-classification-of-fast-acting-therapy-for-patients-at-high-risk-for-macrovascular-events-macrovascular-disease-therapeutic-potential-of-cepcs/

Lev-Ari, A. (2012a). Resident-cell-based Therapy in Human Ischaemic Heart Disease: Evolution in the PROMISE of Thymosin beta4 for Cardiac Repair

http://pharmaceuticalintelligence.com/2012/04/30/93/

Lev-Ari, A. (2012b). Triple Antihypertensive Combination Therapy Significantly Lowers Blood Pressure in Hard-to-Treat Patients with Hypertension and Diabetes

http://pharmaceuticalintelligence.com/2012/05/29/445/

Lev-Ari, A. (2012h). Macrovascular Disease – Therapeutic Potential of cEPCs: Reduction Methods for CV Risk

http://pharmaceuticalintelligence.com/2012/07/02/macrovascular-disease-therapeutic-potential-of-cepcs-reduction-methods-for-cv-risk/

Lev-Ari, A. (2012xx). Coronary artery disease in symptomatic patients referred for coronary angiography: Predicted by Serum Protein Profiles

http://pharmaceuticalintelligence.com/2012/12/29/coronary-artery-disease-in-symptomatic-patients-referred-for-coronary-angiography-predicted-by-serum-protein-profiles/

Lev-Ari, A. (2013a) forthcoming, based on:

Part III: (2006c) Biomarker for Therapeutic Targets of Cardiovascular Risk Reduction by cEPCs Endogenous Augmentation using New Combination Drug Therapy of Three Drug Classes and Several Drug Indications. Northeastern University, Boston, MA 02115

Special Considerations in Blood Lipoproteins, Viscosity, Assessment and Treatment Larry Bernstein

New Insights on Nitric Oxide donors – Part IV Larry Bernstein

The Essential Role of Nitric Oxide and Therapeutic NO Donor Targets in Renal Pharmacotherapy Larry Bernstein

A second look at the transthyretin nutrition inflammatory conundrum Larry Bernstein

What is the role of plasma viscosity in hemostasis and vascular disease risk? Larry Bernstein

Biochemistry of the Coagulation Cascade and Platelet Aggregation – Part I Larry Bernstein

Laboratory, Innovative Technology, Therapeutics Larry Bernstein

Ubiquinin-Proteosome pathway, autophagy, the mitochondrion, proteolysis and cell apoptosis Larry Bernstein

Overview of new strategy for treatment of T2DM: SGLT2 inhibiting oral antidiabetic agents aviralvatsa

Mitochondrial dynamics and cardiovascular diseases ritusaxena

Nitric Oxide and it’s impact on Cardiothoracic Surgery tildabarliya

Telling NO to Cardiac Risk sjwilliamspa

Read Full Post »

CABG or PCI: Patients with Diabetes – CABG Rein Supreme

Posted in Bio Instrumentation in Experimental Life Sciences Research, CABG, Cardiac & Vascular Repair Tools Subsegment, Frontiers in Cardiology and Cardiovascular Disorders, Medical Devices R&D and Inventions, Origins of Cardiovascular Disease, PCI, Pharmacotherapy of Cardiovascular Disease, Regulated Clinical Trials: Design, Methods, Components and IRB related issues, Stents & Tools, tagged CABG, Coronary artery bypass surgery, Coronary artery disease, Drug-eluting stent, National Heart Lung and Blood Institute, Percutaneous coronary intervention, Stanford University School of Medicine on November 5, 2012| 8 Comments »

CABG or PCI: Patients with Diabetes – CABG Rein Supreme

Reporter: Aviva Lev-Ari, PhD, RN

VIEW VIDEO

105

Compelling Evidence for Coronary-Bypass Surgery in Patients with Diabetes

Mark A. Hlatky, M.D.

November 4, 2012DOI: 10.1056/NEJMe1212278

Seventeen years ago, the National Heart, Lung, and Blood Institute issued a clinical alert1 that coronary-artery bypass grafting (CABG) had better rates of survival than percutaneous coronary intervention (PCI) in patients with diabetes. The alert was based on the results of the Bypass Angioplasty Revascularization Investigation (BARI) trial,2 in which patients with multivessel coronary artery disease were randomly assigned to undergo either CABG or PCI.

This recommendation has been controversial ever since, largely because subsequent trials comparing CABG and PCI have enrolled only small numbers of patients with diabetes. A pooled analysis of 10 randomized trials involving 1233 patients with diabetes confirmed that such patients had a particular survival advantage after CABG, as compared with PCI.3 But this evidence was discounted because drug-eluting stents were not used in PCI procedures in the earlier trials, and more recent trials in which drug-eluting stents were used4,5 enrolled relatively few patients with diabetes. Settling this controversy would require a trial with a large number of patients with both diabetes and multivessel coronary artery disease in whom CABG or PCI would be performed with the use of contemporary methods.

Farkouh et al.6 now report in the Journal the results of the definitive Future Revascularization Evaluation in Patients with Diabetes Mellitus: Optimal Management of Multivessel Disease (FREEDOM) trial, in which 1900 patients with diabetes (about as many patients with diabetes as in all previous trials combined) were randomly assigned to undergo either CABG or PCI with drug-eluting stents.

As a cardiologist who does not perform either procedure, I find that the FREEDOM trial provides compelling evidence of the comparative effectiveness of CABG versus PCI in patients with diabetes and multivessel coronary artery disease. After 5 years of follow-up, the 947 patients assigned to undergo CABG had significantly lower mortality (10.9% vs. 16.3%) and fewer myocardial infarctions (6.0% vs. 13.9%) than the 953 patients assigned to undergo PCI. However, patients in the CABG group had significantly more strokes (5.2% vs. 2.4%), mostly because of strokes that occurred within 30 days after revascularization. In the CABG group, the primary composite outcome of death, myocardial infarction, or stroke over 5 years was reduced by 7.9 percentage points, or a relative decrease of 30%, as compared with PCI (18.7% vs. 26.6%, P=0.005). These results are consistent with the findings of multiple previous trials comparing CABG and PCI in patients with diabetes,3 as well as the most recent trials in which drug-eluting stents were used during PCI.4,5

Despite the results of BARI and other trials, over time more and more patients with diabetes have undergone PCI rather than CABG to treat multivessel coronary disease.7,8 The reasons for this trend are uncertain, yet there are two broad potential explanations. First, because PCI technology continues to evolve, many cardiologists simply have dismissed the results of earlier randomized studies as outdated because they used earlier techniques. This is a catch-22, since long-term studies are needed to compare hard outcomes, but evidence from long-term studies may be ignored if therapies are evolving. The results of the FREEDOM trial suggest that the comparative effectiveness of CABG and PCI on hard outcomes remains similar whether PCI is performed without stents, with bare-metal stents, or with drug-eluting stents. Mortality has been consistently reduced by CABG, as compared with PCI, in more than 4000 patients with diabetes who have been evaluated in 13 clinical trials. The controversy should finally be settled.

Another potential reason for the increasing use of PCI in patients with multivessel coronary disease is that the clinical-decision pathway leads patients toward PCI over alternative treatments. Many PCIs today are ad hoc procedures, performed at the time of diagnostic coronary angiography, with the same physician making the diagnosis, recommending the treatment, and performing the procedure. There is little time for informed discussion about alternative treatment options, either medical therapy on the one hand or CABG on the other. Well-informed patients might choose any of those options on the basis of their concerns about the various outcomes of treatment, such as survival, stroke, myocardial infarction, angina, and recovery time. This is a complicated decision, and clinical guidelines in the United States9 and Europe10 now emphasize the importance of more deliberate decision making about coronary revascularization, including discussions with a multidisciplinary heart team.

The results of the FREEDOM trial suggest that patients with diabetes ought to be informed about the potential survival benefit from CABG for the treatment of multivessel disease. These discussions should begin before coronary angiography in order to provide enough time for the patient to digest the information, discuss it with family members and members of the heart team, and come to an informed decision.

Disclosure forms provided by the author are available with the full text of this article at NEJM.org.

This article was published on November 4, 2012, at NEJM.org.

SOURCE INFORMATION

From Stanford University School of Medicine, Stanford, CA.

REFERENCES:

REFERENCES

National Heart, Lung, and Blood Institute (NHLBI). Clinical alert: bypass over angioplasty for patients with diabetes. US National Library of Medicine, National Institutes of Health, September 21, 1995 (http://www.nlm.nih.gov/databases/alerts/bypass_diabetes.html).
The Bypass Angioplasty Revascularization Investigation (BARI) Investigators. Comparison of coronary bypass surgery with angioplasty in patients with multivessel disease. N Engl J Med 1996;335:217-225[Erratum, N Engl J Med 1997;336:147.]Full Text | Web of Science
Hlatky MA, Boothroyd DB, Bravata DM, et al. Coronary artery bypass surgery compared with percutaneous coronary interventions for multivessel disease: a collaborative analysis of individual patient data from ten randomised trials. Lancet 2009;373:1190-1197CrossRef | Web of Science | Medline
Kappetein AP, Feldman TE, Mack MJ, et al. Comparison of coronary bypass surgery with drug-eluting stenting for the treatment of left main and/or three-vessel disease: 3-year follow-up of the SYNTAX trial. Eur Heart J 2011;32:2125-2134CrossRef | Web of Science
Hall R. Coronary Artery Revascularisation in Diabetes trial: five year follow-up data. ESC Clinical Trial and Registry update, Munich, August 27, 2012 (http://www.escardio.org/congresses/esc-2012/congress-reports/Pages/710-5-CARDia.aspx).
Farkouh ME, Domanski M, Sleeper LA, et al. Strategies for multivessel revascularization in patients with diabetes. N Engl J Med 2012. DOI: 10.1056/NEJMoa1211585.
Hassan A, Newman A, Ko DT, et al. Increasing rates of angioplasty versus bypass surgery in Canada, 1994-2005. Am Heart J 2010;160:958-965CrossRef | Web of Science
Frutkin AD, Lindsey JB, Mehta SK, et al. Drug-eluting stents and the use of percutaneous coronary intervention among patients with class I indications for coronary artery bypass surgery undergoing index revascularization: analysis from the NCDR (National Cardiovascular Data Registry). JACC Cardiovasc Interv 2009;2:614-621CrossRef | Web of Science
Hillis LD, Smith PK, Anderson JL, et al. 2011 ACCF/AHA guideline for coronary artery bypass graft surgery: a report of the American College of Cardiology Foundation/American Heart Association Task Force on Practice Guidelines: developed in collaboration with the American Association for Thoracic Surgery, Society of Cardiovascular Anesthesiologists and Society of Thoracic Surgeons. J Am Coll Cardiol 2011;58:e123-e210CrossRef | Web of Science
Wijns W, Kolh P, Danchin N, et al. Guidelines on myocardial revascularization. Eur Heart J2010;31:2501-2555CrossRef | Web of Science | Medline

SOURCE:

http://www.nejm.org/doi/full/10.1056/NEJMe1212278?query=OF

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To Stent or Not? A Critical Decision, Aviva Lev-Ari, PhD, RN

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To Stent or Not? A Critical Decision

Posted in Bio Instrumentation in Experimental Life Sciences Research, CABG, Cardiac & Vascular Repair Tools Subsegment, FDA Regulatory Affairs, Frontiers in Cardiology and Cardiovascular Disorders, Health Economics and Outcomes Research, HTN, Medical Devices R&D and Inventions, Medical Devices R&D Investment, Pharmaceutical Analytics, Pharmacotherapy of Cardiovascular Disease, Regulated Clinical Trials: Design, Methods, Components and IRB related issues, Stents & Tools, Technology Transfer: Biotech and Pharmaceutical on October 23, 2012| 19 Comments »

To Stent or Not? A Critical Decision

Reporter: Aviva Lev-Ari, PhD, RN

VIEW VIDEO – Short Overview [1:45 minutes]

FAME and FAME 2

VIEW VIDEO – Clinical Results [44-54 minutes]

Clinical Results

Clinical Summary

Fractional Flow Reserve-Guided PCI versus Medical Therapy in Stable Coronary Disease

(The FAME II Study)

A Multicenter, Randomized Prospective Study in Consecutive Patients.

This study is sponsored by St. Jude Medical.

Coordinating Clinical Investigator: Bernard De Bruyne, OLV Ziekenhuis, Aalst, Belgium

Fractional Flow Reserve–Guided PCI versus Medical Therapy in Stable Coronary Disease

Bernard De Bruyne, M.D., Ph.D., Nico H.J. Pijls, M.D., Ph.D., Bindu Kalesan, M.P.H., Emanuele Barbato, M.D., Ph.D., Pim A.L. Tonino, M.D., Ph.D., Zsolt Piroth, M.D., Nikola Jagic, M.D., Sven Möbius-Winkler, M.D., Gilles Rioufol, M.D., Ph.D., Nils Witt, M.D., Ph.D., Petr Kala, M.D., Philip MacCarthy, M.D., Thomas Engström, M.D., Keith G. Oldroyd, M.D., Kreton Mavromatis, M.D., Ganesh Manoharan, M.D., Peter Verlee, M.D., Ole Frobert, M.D., Nick Curzen, B.M., Ph.D., Jane B. Johnson, R.N., B.S.N., Peter Jüni, M.D., and William F. Fearon, M.D. for the FAME 2 Trial Investigators

N Engl J Med 2012; 367:991-1001 September 13, 2012DOI: 10.1056/NEJMoa1205361

BACKGROUND

The preferred initial treatment for patients with stable coronary artery disease is the best available medical therapy. We hypothesized that in patients with functionally significant stenoses, as determined by measurement of fractional flow reserve (FFR), percutaneous coronary intervention (PCI) plus the best available medical therapy would be superior to the best available medical therapy alone.

METHODS

In patients with stable coronary artery disease for whom PCI was being considered, we assessed all stenoses by measuring FFR. Patients in whom at least one stenosis was functionally significant (FFR, ≤0.80) were randomly assigned to FFR-guided PCI plus the best available medical therapy (PCI group) or the best available medical therapy alone (medical-therapy group). Patients in whom all stenoses had an FFR of more than 0.80 were entered into a registry and received the best available medical therapy. The primary end point was a composite of death, myocardial infarction, or urgent revascularization.

RESULTS

Recruitment was halted prematurely after enrollment of 1220 patients (888 who underwent randomization and 332 enrolled in the registry) because of a significant between-group difference in the percentage of patients who had a primary end-point event: 4.3% in the PCI group and 12.7% in the medical-therapy group (hazard ratio with PCI, 0.32; 95% confidence interval [CI], 0.19 to 0.53; P<0.001). The difference was driven by a lower rate of urgent revascularization in the PCI group than in the medical-therapy group (1.6% vs. 11.1%; hazard ratio, 0.13; 95% CI, 0.06 to 0.30; P<0.001); in particular, in the PCI group, fewer urgent revascularizations were triggered by a myocardial infarction or evidence of ischemia on electrocardiography (hazard ratio, 0.13; 95% CI, 0.04 to 0.43; P<0.001). Among patients in the registry, 3.0% had a primary end-point event.

CONCLUSIONS

In patients with stable coronary artery disease and functionally significant stenoses, FFR-guided PCI plus the best available medical therapy, as compared with the best available medical therapy alone, decreased the need for urgent revascularization. In patients without ischemia, the outcome appeared to be favorable with the best available medical therapy alone. (Funded by St. Jude Medical; ClinicalTrials.gov number, NCT01132495.)

Supported by St. Jude Medical.

Disclosure forms provided by the authors are available with the full text of this article at NEJM.org.

This article was published on August 28, 2012, and updated on October 18, 2012, at NEJM.org.

SOURCE INFORMATION

From the Cardiovascular Center Aalst, Onze-Lieve-Vrouw Clinic, Aalst, Belgium (B.D.B., E.B.); Department of Cardiology, Catharina Hospital, and Department of Biomedical Engineering, Eindhoven University of Technology — both in Eindhoven, the Netherlands (N.H.J.P., P.A.L.T.); Division of Clinical Epidemiology and Biostatistics, Institute of Social and Preventive Medicine and Clinical Trials Unit Bern, University of Bern, Bern, Switzerland (B.K., P.J.); Hungarian Institute of Cardiology, Budapest (Z.P.); Clinical Center Kragujevac, Kragujevac, Serbia (N.J.); Heart Center Leipzig, Leipzig, Germany (S.M.-W.); Cardiovascular Hospital, Lyon, France (G.R.); Södersjukhuset, Stockholm (N.W.), and Karolinska Institutet at Örebro University Hospital, Örebro (O.F.) — both in Sweden; Department of Internal Medicine and Cardiology, University Hospital Brno, Brno, Czech Republic (P.K.); King’s College Hospital, London (P.M.), Golden Jubilee National Hospital, Glasgow (K.G.O.), Royal Victoria Hospital, Belfast (G.M.), and Department of Cardiology, Southampton University Hospital Trust, Southampton (N.C.) — all in the United Kingdom; Department of Cardiology, Rigshospitalet University Hospital, Copenhagen (T.E.); Atlanta Veterans Affairs Medical Center, Atlanta (K.M.); Northeast Cardiology Associates, Bangor, ME (P.V.); St. Jude Medical, Plymouth, MN (J.B.J.); and Stanford University Medical Center, Stanford, CA (W.F.F.).

Address reprint requests to Dr. De Bruyne at the Cardiovascular Centre Aalst, OLV-Clinic, Moorselbaan 164, B-9300 Aalst, Belgium, or atbernard.de.bruyne@olvz-aalst.be.

The investigators in the Fractional Flow Reserve versus Angiography for Multivessel Evaluation 2 (FAME 2) trial are listed in the Supplementary Appendix, available at NEJM.org.

Conclusions

The FAME II study results show that FFR-guided PCI compared to medical management alone significantly reduces patients’ risk for unplanned hospital readmission with urgent revascularization.

The new data support the paradigm of “Functionally Complete Revascularization,” that is, stenting of ischemic lesions and medical treatment of non-ischemic ones.

Routine Use of Ffr Significantly Improves the Outcome of Treatment in Stable CAD Patients. St. Jude Medical is focused on reducing risk by continuously finding ways to put more control into the hands of those who save and enhance lives.

SUMMARY OF KEY FINDINGS

FFR significantly improves outcome of treatment in stable patients. The results of FAME II, a St. Jude Medical sponsored clinical trial, show a significant benefit in using FFR-guided intervention. In patients with stable coronary artery disease undergoing PressureWireTM-guided intervention, PCI plus medical therapy was found to improve outcomes compared to medical therapy alone.

FFR Significantly Reduces Risk of Unplanned Hospital Readmission for Urgent Revascularization

Background

In patients with clinically stable coronary disease, PCI has not been shown to affect clinical outcomes such as death, nonfatal myocardial infarction and the need for urgent revascularization. In previous trials on revascularization, treatment has been guided by the angiographic appearance of the lesions. It is likely that in all previous trials dealing with patients with nonacute coronary artery disease (CAD), a sizable proportion of patients did not have ischemia.

Objectives

The overall purpose of the FAME II study was to compare the clinical outcomes of FFR-guided contemporary PCI plus medical therapy versus medical therapy alone in patients with stable coronary disease.

Methods

The FAME II trial is a prospective, multicenter randomized clinical trial with an all comers design. All consecutive patients with stable clinical condition and angiographically defined one-, two- or three-vessel coronary artery disease and amenable for PCI were screened and considered for participation in the study. Patients with at least one hemodynamically significant lesion were randomized into PCI (drug-eluting stents [DES] were recommended) plus medical therapy or medical therapy alone. It was expected that in approximately 20% of patients no stenoses would be hemodynamically significant.

Patients without hemodynamically significant lesions were enrolled in the registry portion of the study and treated with medical therapy. For prospectively collected data in the randomized study and the registry, an independent clinical events committee (CEC) adjudicated all clinical endpoints.

Key Exclusion Criteria

 Prior coronary artery bypass grafting (CABG)

 Left ventricular ejection fraction (LVEF) <30%

 Left main (LM) stenosis

For patients with one or more significant lesions, there was an 86% relative reduction in the risk for unplanned hospital readmission with urgent revascularization for patients who received FFR-guided PCI plus medical therapy.

These findings support FFR-guided PCI compared to medical management alone to improve outcomes in the treatment of stable patients with single-vessel or multivessel coronary artery disease.

Study Endpoints

Original FAME II Study Flow Chart Primary Endpoint Composite of:

 all-cause death

 nonfatal myocardial infarction

 unplanned hospitalization with urgent revascularization

As adjudicated by an independent CEC.

Secondary Endpoints

 Individual components of the primary endpoint*

 Cardiac death*

 Nonurgent revascularization procedures*

 Angina class

*As adjudicated by an independent CEC.

Stable patients scheduled for 1, 2 or 3 vessel DES stenting

RANDOMIZED TRIAL REGISTRY

FFR in all target lesions

Randomization 1:1

PCI + medical therapy medical therapy

Follow-up after 1, 6 months, 1, 2, 3, 4 and 5 years

At least 1 stenosis with FFR ≤ 0.80 When all FFR > 0.80

Medical Therapy

 Aspirin

 Beta blocker

 Calcium blocker and/or nitrate as necessary

 Statin

 ACE inhibitor (or ARB)

 Diabetes treatment guided by a specialist

FFR-guided PCI

 FFR measured during hyperemia

 PCI only if FFR ≤ 0.80 and randomized to PCI

 2nd generation drug-eluting stents (recommended)

Fractional Flow Reserve Measurements Intracoronary pressure measurements were obtained with a guiding catheter (fluid-filled) and the St. Jude Medical PressureWire CertusTM or AerisTM guidewire.

Results

The independent Data and Safety Monitoring Board recommended halting patient recruitment due to a significantly increased patient risk of major adverse cardiac events among patients randomized to medical therapy alone compared to patients randomized to medical therapy plus PCI.

The enrollment goal in FAME II was approximately 1,800 patients (randomized study and registry combined). The data sample presented here is the same data on which the decision to halt enrollment was based (January 15, 2012).

A total of 888 (73%) patients with ischemic lesions had been successfully randomized, and an additional 332 (27%) patients were enrolled in the registry because no ischemic lesions were detected. In total, 1,220 patients were enrolled in the FAME II trial, including 1,054 who were assigned to follow-up.

Medical Therapy

Actual FAME II Study Flow Chart

* Note that 6 patients had total occlusions supplying akinetic myocardium and were therefore not considered for PCI; 1 patient had 2 FFR negative lesions and was therefore included in the registry, however, a subsequently detected total occlusion was eventually treated with DES.

Randomized (n = 888)

Underwent FFR (n = 1220)

FFR >0.80 in all lesions included in registry

(n = 332)*

Allocated to medical therapy alone (n = 441)

Received allocated intervention (n = 439)

Did not receive allocated intervention (n = 2)

Erroneously received DES (n = 2)

Randomly selected to receive follow-up (n = 166)

Received medical therapy alone (n = 165)

Received DES (n = 1)

Allocated to PCI+medical therapy (n = 447)

Received allocated intervention (n = 435)

Did not receive allocated intervention (n = 12)

Treated with balloon angioplasty (n = 3)

Underwent CABG rather than PCI (n = 4)

Received medical therapy, planned for staged

procedure (n = 3)

Received medical therapy, unsuccessful PCI (n = 1)

Received medical therapy, FFR >0.8 (n = 1)

Follow-up information for primary endpoint

available until Jan 15, 2012 (n = 446)

Followed up and alive (n = 445)

Deceased (n = 1)

Follow-up at Jan 15, 2012 unavailable (n = 1)

Withdrew (n = 1)

Lost to follow-up (n = 0)

Follow-up information for primary endpoint

available until Jan 15, 2012 (n = 439)

Followed up and alive (n = 436)

Deceased (n = 3)

Follow-up at Jan 15, 2012 unavailable (n = 2)

Withdrew (n = 2)

Lost to follow-up (n = 0)

Follow-up information for primary endpoint

available until Jan 15, 2012 (n = 163)

Followed up and alive (n = 163)

Deceased (n = 0)

Follow-up at Jan 15, 2012 unavailable (n = 3)

Withdrew (n = 1)

Lost to follow-up (n = 2)

Analyzed on primary clinical endpoint (n = 166)

Censored at time of lost to follow-up

or withdrawal (n = 3)

Analyzed on primary clinical endpoint (n = 441)

Censored at time of lost to follow-up

or withdrawal (n = 2)

Analyzed on primary clinical endpoint (n = 447)

Censored at time of lost to follow-up

or withdrawal (n = 1)

Patients n = 447 n = 441 n = 166

Age in years, mean±SD 63.52 ± 9.35 63.86 ± 9.62 63.58 ± 9.75 0.90

Men, n (%) 356 (79.6) 338 (76.6) 113 (68.1) 0.005

BMI, mean±SD 28.29 ± 4.27 28.44 ± 4.55 27.83 ± 3.94 0.14

Family history of coronary artery disease, n (%) 216 (48.3) 207 (46.9) 76 (45.8) 0.65

Current smoking, n (%) 89 (19.9) 90 (20.4) 35 (21.1) 0.79

Hypertension, n (%) 347 (77.6) 343 (77.8) 136 (81.9) 0.23

Hypercholesterolemia, n (%) 330 (73.9) 348 (78.9) 118 (71.1) 0.15

Diabetes mellitus, n (%) 123 (27.5) 117 (26.5) 42 (25.3) 0.65

Insulin requiring diabetes, n (%) 39 (8.7) 39 (8.8) 10 (6.0) 0.24

Renal insufficiency (Creatinine > 2.0 mg/dL), n (%) 8 (1.8) 12 (2.7) 7 (4.2) 0.14

Peripheral vascular disease, n (%) 43 (9.6) 47 (10.7) 8 (4.8) 0.065

History of stroke/TIA, n (%) 33 (7.4) 28 (6.3) 10 (6.0) 0.69

History of MI, n (%) 164 (37.2) 165 (37.8) 60 (36.6) 0.83

History of PCI in target vessel, n (%) 80 (17.9) 76 (17.2) 34 (20.5) 0.37

Angina Class, n (%) 0.64

Asymptomatic 53 (11.9) 46 (10.5) 17 (10.2) .

CCS class I 82 (18.3) 98 (22.3) 42 (25.3) .

CCS class II 204 (45.6) 197 (44.8) 74 (44.6) .

CCS class III 80 (17.9) 65 (14.8) 23 (13.9) .

CCS IV, stabilized 28 (6.3) 34 (7.7) 10 (6.0) .

Silent Ischemia, n (%) 73 (16.3) 73 (16.6) 27 (16.3) 0.96

Left ventricular ejection fraction<50%, n (%) 83 (19.6) 56 (13.7) 27 (18.0) 0.69

Classification of patients according to angiography

No. of significant lesions per patient, mean±SD 1.87 ± 1.05 1.73 ± 0.94 1.32 ± 0.59 <0.001

No. of vessels per patient with at least one significant lesion, n (%) <0.001

1 251 (56.2) 261 (59.2) 136 (81.9) .

2 156 (34.9) 146 (33.1) 26 (15.7) .

3 40 (8.9) 34 (7.7) 4 (2.4) .

Proximal or mid LAD stenosis (%) 65.1 62.6 44.6 <0.001

Classification of patients according to FFR

No. of significant lesions per patient according to FFR, mean±SD 1.52 ± 0.78 1.42 ± 0.73 0.03 ± 0.17 <0.001

No. of vessels with significant lesions by FFR, n (%) 1.00

1 331 (74.0) 343 (77.8) 3.0

2 102 (22.8) 85 (19.3) 0 (0)

3 14 (3.1) 13 (2.9) 0 (0)

Proximal or mid LAD stenosis (%) 62.4 59.6 0.6 <0.001

Lesions n = 890 n = 815 n = 241

Classification of lesions according to angiography .

No. of significant lesions (diameter stenosis>50%), n (%) 837 (94.0) 764 (93.7) 219 (90.9) 0.13

Percent diameter stenosis, n (%) <0.001

<50% 53 (6.0) 51 (6.3) 22 (9.1)

50-69% 317 (35.6) 331 (40.6) 176 (73.0)

70-90% 383 (43.0) 331 (40.6) 38 (15.8)

>90% 101 (11.3) 80 (9.8) 0 (0)

Total occlusions 36 (4.0) 22 (2.7) 5 (2.1)

Classification of lesions according to FFR

No. of significant lesions (FFR≤0.80), n (%) 679 (76.3) 625 (76.7) 5* (2.1) <0.001

FFR in significant lesions, mean±SD 0.68 ± 0.10 0.68 ± 0.15 0.50 ± 0.00 0.013

Randomized Trial Registry p-value for

Trial vs. Registry

PCI+medical therapy medical therapy alone

**Differences between the two randomized groups were not significant with the exception of left ventricular ejection fraction<50% (p<0.05). Data are mean±SD or number of patients assessed (%). P-value using chi square test;

when cells are small Fisher’s test is used. Data for ejection fraction were available for 423 in PCI&medical therapy, 410 in medical therapy and 150 in registry. Data for history of MI were available for 442 in PCI&medical therapy,

436 in medical therapy and 295 in registry. CCS=Canadian Cardiovascular Society functional classification of angina pectoris; Data available in 447 in PCI&medical therapy, 440 in medical therapy, and 166 in registry. **5 totally

occluded arteries supplied infarcted areas and therefore not considered for revascularization using PCI. In patient level analysis p-value calculated using chi-square test, in case of cells <15 Fisher’s test. In lesion level analysis,

mixed maximum-likelihood logistic regression models were used for comparisons between groups for dichotomous variables and mixed maximum-likelihood linear regression models for continuous variables to account for the

correlation of multiple lesions within patients.

Conclusions

The FAME II study results show that FFR-guided PCI compared to medical management alone significantly reduces patients’ risk for unplanned hospital readmission with urgent revascularization.

The new data support the paradigm of “Functionally Complete Revascularization,” that is, stenting of ischemic lesions and medical treatment of non-ischemic ones.

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ATRIAL FIBRILLATION CARDIAC RHYTHM MANAGEMENT CARDIOVASCULAR NEUROMODULATION

The content of this clinical summary is based on:

 De Bruyne, B., et al. Fractional Flow Reserve-Guided Percutaneous Coronary Intervention Versus Medical Treatment in Stable Coronary Disease,

N Engl J Med 2012; published online ahead of print August 28, 2012.

 http://www.Clinicaltrials.gov. FAME II Study Identifier: NCT01132495.

 FAME II study protocol (on file, St. Jude Medical).

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Outcomes in High Cardiovascular Risk Patients: Prasugrel (Effient) vs. Clopidogrel (Plavix); Aliskiren (Tekturna) added to ACE or added to ARB

Posted in CABG, Cell Biology, Signaling & Cell Circuits, Chemical Biology and its relations to Metabolic Disease, Disease Biology, Small Molecules in Development of Therapeutic Drugs, FDA Regulatory Affairs, Frontiers in Cardiology and Cardiovascular Disorders, Health Economics and Outcomes Research, Health Law & Patient Safety, HTN, Origins of Cardiovascular Disease, Pharmaceutical Industry Competitive Intelligence, Pharmaceutical R&D Investment, Pharmacotherapy of Cardiovascular Disease, Regulated Clinical Trials: Design, Methods, Components and IRB related issues, tagged American College of Cardiology, Antiplatelet drug, Clopidogrel, Coronary artery bypass surgery, Daiichi Sankyo, Eli Lilly, European Society of Cardiology, myocardial infarction, New England Journal of Medicine, Prasugrel, ST elevation, Ticagrelor on August 27, 2012| 7 Comments »

Reporter and Curator: Aviva Lev-Ari, PhD, RN

WOEST (What is the Optimal Antiplatelet and Anticoagulant Therapy in Patients with Oral Anticoagulantion and Coronary Stenting): Get Rid Of The Aspirin In Triple Therapy

According to current guidelines and clinical practice, PCI patients already taking an oral anticoagulant generally end up on triple therapy comprising the anticoagulant plus clopidogrel and aspirin. However, there is no supporting evidence base for this approach and the triple therapy regimen is known to increase bleeding complications. Now a new study– the first randomized trial to address this situation, according to the investigators– may have a large impact on clinical practice by demonstrating that the omission of aspirin in this context appears to be safe and may reduce adverse events.

Results of the WOEST (What is the Optimal Antiplatelet and Anticoagulant Therapy in Patients with Oral Anticoagulantion and Coronary Stenting) trial were presented by Willem Dewilde at the ESC in Munich today. Investigators in the Netherlands and Belgium randomized 573 patients to triple therapy or dual therapy of an anticoagulant plus clopidogrel for at least one month after implantation of a bare-metal stent or one year after a drug-eluting stent. Two-thirds of the patients were receiving oral anticoagulation for atrial fibrillation.

The primary endpoint, the total number of bleeding events, was dramatically reduced in the dual therapy group at one year:

44.9% in the triple therapy group versus 19.5% (HR 0.36, CI 0.26-0.50)

There were 3 intracranial bleeds in each group. Most of the difference in bleeding occurred in TIMI minor and minimal bleeding. The difference in TIMI major bleeding (3.3% versus 5.8%) did not achieve statistical significance.

Clinical events, the trials’s secondary endpoint, were numerically lower in the dual therapy group. The difference in mortality achieved statistical significance.

Mortality: 7 deaths (2.6%) in the dual therapy group versus 18 deaths (6.4%) in the triple therapy group, p=0.027
MI: 3.3% versus 4.7%, p=0.382
TVR: 7.3% versus 6.8%, p=0.876
Stroke: 1.1% versus 2.9%, p=0.128)
Stent thrombosis: 1.5% versus 3.2%, p=0.165

“The WOEST study demonstrates that omitting aspirin leads to less bleedings but does not increase the risk of stent thrombosis, stroke or myocardial infarction,” said Dewilde in an ESC press release. “Although the number of patients in the trial is limited, this is an important finding with implications for future treatment and guidelines in this group of patients known to be at high risk of bleeding and thrombotic complications.”

David Holmes said the trial addressed “an incredibly important issue” and predicted that it would “change the way we practice medicine, it will change practice right away.” Keith Fox said that the evidence base prior to WOEST was extremely limited and that the trial showed that there was no hazard in doing without aspirin. The ESC discussant, Marco Valgimigli, said the trial showed it was safe to drop aspirin and provided another demonstration that “we have hit the wall” with anticoagulation.

Republished with permission from CardioExchange, a NEJM group publication.

http://www.forbes.com/sites/larryhusten/2012/08/28/woest-get-rid-of-the-aspirin-in-triple-therapy/

European Society of Cardiology: Prasugrel Can’t Top Clopidogrel in ACS

By Todd Neale, Senior Staff Writer, MedPage Today

Published: August 26, 2012

Reviewed by Robert Jasmer, MD; Associate Clinical Professor of Medicine, University of California, San Francisco

MUNICH — For patients with unstable angina or non-ST-segment elevation myocardial infarction (non-STEMI) who do not undergo revascularization, increasing platelet inhibition may not improve outcomes, a randomized trial showed.

Added to a background of low-dose aspirin, prasugrel (Effient) did not significantly reduce the rate of MI, stroke, or cardiovascular death compared with clopidogrel (13.9% versus 16%, HR 0.91, 95% CI 0.79 to 1.05), according to Matthew Roe, MD, of Duke University in Durham, N.C.

The risk of severe bleeding was similar with both drugs, although minor and moderate bleeding were increased with prasugrel, Roe reported at the European Society of Cardiology meeting here. The findings were published simultaneously online in the New England Journal of Medicine.

“I think the outcome is a bit surprising because we think usually that more aggressive antiplatelet therapy, conceivably, in the face of an acute coronary syndrome and non-ST-elevation would lead to lesser adverse outcome from acute myocardial infarction or death,” said William Zoghbi, MD, from Methodist DeBakey Heart Center in Houston and president of the American College of Cardiology.

But he said clinicians need to respect the data “and start thinking about pathogenesis and what we’re trying to do with any of our new interventions.”

In patients with unstable angina or non-STEMI, practice guidelines call for angiography within 48 to 72 hours with provisional revascularization. Many of these patients do not ultimately undergo revascularization, placing them at greater risk compared with those who have their arteries opened with percutaneous coronary intervention (PCI) or coronary artery bypass graft (CABG).

Recommended medical therapy is with clopidogrel and aspirin, which is an approach that will not change from the current findings, Zoghbi said.

The purpose of the TRILOGY ACS trial was to explore whether using a more powerful platelet inhibitor — prasugrel — would improve outcomes compared clopidogrel (Plavix) in this high-risk patient subset.

The primary analysis involved 7,243 patients younger than 75 (mean age 62) who were receiving aspirin and were randomized to prasugrel 10 mg daily (or 5 mg daily for those weighing less than 132 pounds) or to clopidogrel 75 mg daily. The researchers recommended a daily aspirin dose of 100 mg or less.

A secondary, exploratory analysis involved 2,083 patients, 75 or older, who were randomized to prasugrel 5 mg daily or to clopidogrel 75 mg daily.

The lack of efficacy seen in the primary analysis of patients younger than 75 remained when patients of all ages were combined. There were no between-group differences for any of the components of the primary endpoint.

A prespecified secondary analysis taking multiple recurrent ischemic events into consideration showed a lower risk of MI, stroke, and cardiovascular death with prasugrel in the younger patients (HR 0.85, 95% CI 0.72 to 1.00, P=0.04), a finding consistent with the main results of the TRITON-TIMI 38 trial, which involved patients treated with PCI. The apparent benefit appeared after 12 months of treatment.

“Although this observation is exploratory, it raises the question of whether investigation of the multiplicity of ischemic events is warranted in future secondary-prevention trials, rather than solely analyzing the time to the first event, as has been traditional in studies involving patients who have had an acute coronary event,” the researchers wrote.

Rates of GUSTO severe or life threatening bleeding and TIMI major bleeding — as well as intracranial hemorrhage — were similar in the two groups in both the younger patients and in the overall study population. When minor and moderate bleeding events were added, the bleeding rate was higher with prasugrel.

There were no widespread differences between the groups in rates of nonhemorrhagic serious adverse events, but heart failure was more frequent with clopidogrel (1.8% versus 1.3%, P=0.045).

Douglas Weaver, MD, of Henry Ford Health System, said that he does not think the findings will have any impact on the use of prasugrel, which is not indicated for the patient population included in the study.

“It just doesn’t pass muster in improving value over clopidogrel,” said Weaver, a past president of the American College of Cardiology.

From a clinical perspective, he said, an important message from the study is the evidence of the safety of a reduced dose of prasugrel in the patients 75 and older, which is a consideration when prescribing prasugrel for patients undergoing PCI.

In comments following Roe’s presentation, Raffaele De Caterina, MD, PhD, of the G. d’Annunzio University in Chieti, Italy, provided context about how the findings fit in with the rest of the literature.

He compared the current results to those of a substudy of the PLATO trial, which involved ticagrelor (Brilinta).

In that trial, ticagrelor significantly reduced vascular death, MI, and stroke (HR 0.85, 95% CI 0.73 to 1.00, P=0.045) — the primary endpoint — and all-cause death (HR 0.75, 95% CI 0.61 to 0.93).

He then highlighted the ESC guidelines on treating patients with acute coronary syndromes without persistent ST-segment elevation.

In those, ticagrelor is recommended for all patients at moderate-to-high risk of ischemic events, regardless of initial treatment strategy and including those pre-treated with clopidogrel, and prasugrel is recommended for those who have not taken another P2Y12 inhibitor, who have a known coronary anatomy, and who are proceeding to PCI.

“I believe such statements and recommendations of the guidelines should not be changed,” De Caterina said.

TRILOGY ACS was funded by Eli Lilly and Daiichi Sankyo.

Roe reported relationships with Daiichi Sankyo, Eli Lilly, AstraZeneca, Bristol-Myers Squibb, Janssen Pharmaceuticals, Merck, Hoffmann-La Roche, and sanofi-aventis. The other authors reported numerous relationships with industry.

Primary source: New England Journal of Medicine

Source reference:
Roe M, et al “Prasugrel versus clopidogrel for acute coronary syndromes without revascularization” N Engl J Med2012; DOI: 10.1056/NEJMoa1205512.

http://www.medpagetoday.com/MeetingCoverage/ESCCongress/34375?utm_content=&utm_medium=email&utm_campaign=DailyHeadlines&utm_source=WC&xid=NL_DHE_2012-08-27&eun=g99985d0r&userid=99985&email=avivalev-ari@alum.berkeley.edu&mu_id=5099207

Prematurely halted ALTITUDE trial showed When added to monotherapy with either an ACE inhibitor or an angiotensin receptor blocker (ARB), aliskiren (Tekturna) did not improve outcomes in patients with type 2 diabetes who had high cardiovascular and renal risk

ESC: Aliskiren Onboard No Help in T2D

By Todd Neale, Senior Staff Writer, MedPage Today

Published: August 26, 2012

Reviewed by Robert Jasmer, MD; Associate Clinical Professor of Medicine, University of California, San Francisco

MUNICH — When added to monotherapy with either an ACE inhibitor or an angiotensin receptor blocker (ARB), aliskiren (Tekturna) did not improve outcomes in patients with type 2 diabetes who had high cardiovascular and renal risk, the prematurely halted ALTITUDE trial showed.

Through an average follow-up of 32 months, a composite of various cardiovascular and renal outcomes occurred in 17.9% of patients receiving the direct renin inhibitor and 16.8% of those receiving placebo (HR 1.08, 95% CI 0.98 to 1.20), according to Hans-Henrik Parving, MD, DMSc, of the University of Copenhagen and Aarhus University in Denmark.

As a Hot Line presentation European Society of Cardiology meeting here, Parving reported that there were no significant differences on any of the individual components of the endpoint — cardiovascular death, resuscitated sudden death, MI, stroke, unplanned hospitalization for heart failure, doubling of baseline serum creatinine, and onset of end-stage renal disease — or all-cause death.

The rate of stroke — mostly ischemic stroke — was numerically higher with aliskiren, although the result fell short of statistical significance (3.4% versus 2.8%; HR 1.25, 95% CI 0.98 to 1.60,P=0.07).

Thus, Parving said, using aliskiren with ACE inhibitors or ARBs in these high-risk patients “is not recommended and may even be harmful.”

The data monitoring committee for the ALTITUDE trial decided to stop the study early in December 2011 both for futility and for adverse events. Then, earlier this year, the FDA issued a warning about using aliskiren with ACE inhibitors or ARBs and changed the drug label to reflect a contraindication for such combinations in patients with diabetes or renal impairment.

The trial included 8,561 patients with type 2 diabetes who had a high risk of cardiovascular or renal disease who were randomized to aliskiren — at 150 mg daily for 1 month followed by 300 mg daily thereafter — or placebo in addition to monotherapy with either an ACE inhibitor or an ARB (but not both).

Adding aliskiren did not improve outcomes, and in fact, may have caused harm, Parving said, as indicated by the apparent increase in stroke risk.

He said that could be explained by the impaired autoregulation of patients with diabetes or by chance, as there are no indications of a stroke risk in other studies of the drug.

Johannes Mann, of Friedrich Alexander University in Erlangen, Germany, and McMaster University in Hamilton, Ontario, who served as the discussant following Parving’s presentation, agreed that it could be a chance finding, but said that it could also be a direct effect of aliskiren itself.

He concluded that the stroke risk was not explained, however, by dual renin system inhibition, because such a signal was not seen in the ONTARGET trial, which compared the combination of ramipril (an ACE inhibitor) and telmisartan (an ARB) with each drug as monotherapy.

As noted when the trial was halted last year, adverse events were more frequent in the aliskiren group.

The percentage of patients who had a potassium level of 5.5 to less than 6.0 mmol/L was greater with active treatment (21% versus 16%), as was the percentage of those with a potassium level of 6.0 mmol/L or greater (8.8% versus 5.6%).

Aliskiren carried higher risks of hyperkalemia (38.7% versus 28.6%), hypotension (12.1% versus 8%), diarrhea (9.6% versus 7.2%), and falls (2.8% versus 2.6%). There was one death caused by hyperkalemia.

Douglas Weaver, MD, of the Henry Ford Health System in Detroit, said that the findings were disappointing, but that they likely wouldn’t change how aliskiren is used in practice.

“I don’t think this is going to have a negative or a positive effect on it,” said Weaver, who is a past president of the American College of Cardiology.

ALTITUDE was sponsored by Novartis Pharma AG.

The executive committee and other investigators or their institutions received a consultancy fee. Some of the authors are employees of Novartis and therefore eligible for stock and stock options.

Primary source: European Society of Cardiology
Source reference:
Parving H-H, et al “The Aliskiren Trial in Type 2 Diabetes Using Cardio-Renal Endpoints (ALTITUDE)” ESC 2012; Abstract 399.

http://www.medpagetoday.com/MeetingCoverage/ESCCongress/34388?utm_content=&utm_medium=email&utm_campaign=DailyHeadlines&utm_source=WC&xid=NL_DHE_2012-08-27&eun=g99985d0r&userid=99985&email=avivalev-ari@alum.berkeley.edu&mu_id=5099207

Aliskiren

From Wikipedia, the free encyclopedia

Aliskiren

Systematic (IUPAC) name
(2S,4S,5S,7S)-5-amino-N-(2-carbamoyl-2,2-dimethylethyl)-4-hydroxy-7-{[4-methoxy-3-(3-methoxypropoxy)phenyl]methyl}-8-methyl-2-(propan-2-yl)nonanamide
Aliskiren (INN) (trade names Tekturna, U.S.; Rasilez, U.K. and elsewhere) is the first in a class of drugs called direct renin inhibitors. Its current licensed indication is essential (primary) hypertension.

Aliskiren was co-developed by the Swiss pharmaceutical companies Novartis and Speedel.^[1]^[2] It was approved by the U.S. Food and Drug Administration in 2007 for the treatment of primary hypertension.^[3]

In December 2011, Novartis had to halt a clinical trial of the drug after discovering increased incidence of non-fatal stroke, renal complications, hyperkalemia and hypotension in patients with diabetes and renal impairment.^[4]

The following recommendations are being added to the drug labels for aliskiren-containing products as of 4/20/12:

I) A new contraindication against the use of aliskiren with ARBs or ACEIs in patients with diabetes because of the risk of renal impairment, hypotension, and hyperkalemia. II) A warning to avoid use of aliskiren with ARBs or ACEIs in patients with moderate to severe renal impairment (i.e., where glomerular filtration rate [GFR] < 60 mL/min).

Mechanism of Action

Renin is the first enzyme in the renin-angiotensin-aldosterone system which plays a role in blood pressure control. Renin cleaves angiotensinogen to angiotensin I, which is in turn converted by angiotensin-converting enzyme (ACE) toangiotensin II. Angiotensin II has both direct and indirect effects on blood pressure. It directly causes arterial smooth muscle to contract, leading to vasoconstriction and increased blood pressure. Angiotensin II also stimulates the production of aldosterone from the adrenal cortex, which causes the tubules of the kidneys to increase reabsorption of sodium, with water following thereby increasing plasma volume and blood pressure.

Aliskiren binds to the S3^bp binding pocket of renin, essential for its activity.^[5] Binding to this pocket prevents the conversion of angiotensinogen to angiotensin I.

Aliskiren is also available as combination therapy with hydrochlorothiazide.^[6]

Many drugs control blood pressure by interfering with angiotensin or aldosterone. However, when these drugs are used chronically, the body increases renin production, which drives blood pressure up again. Therefore, doctors have been looking for a drug to inhibit renin directly. Aliskiren is the first drug to do so.^[7]^[8]

Aliskiren may have renoprotective effects that are independent of its blood pressure−lowering effect in patients with hypertension, type 2 diabetes, and nephropathy who are receiving the recommended renoprotective treatment. According to the AVOID study, researchers found that treatment with 300 mg of aliskiren daily, as compared with placebo, reduced the mean urinary albumin-to-creatinine ratio by 20% (95% confidence interval, 9 to 30; P<0.001), with a reduction of 50% or more in 24.7% of the patients who received aliskiren as compared with 12.5% of those who received placebo (P<0.001). Furthermore, the AVOID trial shows that treatment with 300 mg of aliskiren daily reduces albuminuria in patients with hypertension, type 2 diabetes, and proteinuria who are receiving the recommended maximal renoprotective treatment with losartan and optimal antihypertensive therapy. Therefore, direct renin inhibition will have a critical role in strategic renoprotective pharmacotherapy, in conjunction with dual blockade of the renin−angiotensin−aldosterone system with the use of ACE inhibitors and angiotensin II–receptor blockers, very high doses of angiotensin II−receptor blockers, and aldosterone blockade.^[9]

Adverse effects

Angioedema
Hyperkalemia (particularly when used with ACE inhibitors in diabetic patients)
Hypotension (particularly in volume-depleted patients)
Diarrhea and other GI symptoms
Headache
Dizziness
Cough
Rash
Elevated uric acid, gout, and renal stones
Rarely: allergic swelling of the face, lips or tongue and difficulty breathing

Contraindications

Pregnancy: other drugs such as ACE inhibitors, also acting on the renin-angiotensin system have been associated with fetal malformations and neonatal death^[10]
Breast feeding: during animal studies, the drug has been found present in milk.^[10]

Aliskiren has not yet been evaluated in patients with significantly impaired renal function.

Drug interactions

Aliskiren is a minor substrate of CYP3A4 and, more important, P-glycoprotein:

Reduces furosemide blood concentration.
Atorvastatin may increase blood concentration, however no dose adjustment needed.
Possible interaction with ciclosporin (the concomitant use of ciclosporin and aliskiren is contraindicated).
Caution should be exercised when aliskiren is administered with ketoconazole or other moderate P-gp inhibitors (itraconazole, clarithromycin, telithromycin, erythromycin, amiodarone).
Doctors should stop prescribing aliskiren-containing medicines to patients with diabetes (type 1 or type 2) or with moderate to severe kidney impairment who are also taking an ACE inhibitor or ARB, and should consider alternative antihypertensive treatment as necessary.^[11]

References

^ Gradman A, Schmieder R, Lins R, Nussberger J, Chiang Y, Bedigian M (2005). “Aliskiren, a novel orally effective renin inhibitor, provides dose-dependent antihypertensive efficacy and placebo-like tolerability in hypertensive patients”. Circulation 111 (8): 1012–8. doi:10.1161/01.CIR.0000156466.02908.ED. PMID 15723979.
^ Straessen JA, Li Y, and Richart T (2006). “Oral Renin Inhibitors”. Lancet 368 (9545): 1449–56. doi:10.1016/S0140-6736(06)69442-7. PMID 17055947.
^ “First Hypertension Drug to Inhibit Kidney Enzyme Approved”. CBC. 2007-03-06. Retrieved 2007-03-14.^{[dead link]}
^ Healthzone.ca: Blood-pressure drug reviewed amid dangerous side effects
^ “Chemistry & Biology : Structure-based drug design: the discovery of novel nonpeptide orally active inhibitors of human renin”. ScienceDirect. Retrieved 2010-01-20.
^ Baldwin CM, Plosker GL.[1]. doi:10.2165/00003495-200969070-00004. Drugs 2009; 69(7):833-841.
^ Ingelfinger JR (June 2008). “Aliskiren and dual therapy in type 2 diabetes mellitus”. N. Engl. J. Med. 358 (23): 2503–5. doi:10.1056/NEJMe0803375.PMID 18525047.
^ PharmaXChange: Direct Renin Inhibitors as Antihypertensive Drugs
^ Parving HH, Persson F, Lewis JB, Lewis EJ, Hollenberg NK. “Aliskiren Combined with Losartan in Type 2 Diabetes and Nephropathy,” N Engl J Med 2008;358:2433-46.
^ ^a ^b Drugs.com: Tekturna
^ European Medicines Agency recommends new contraindications and warnings for aliskiren-containing medicines.

External links

Prescribing Information for Tekturna
aliskiren at the US National Library of Medicine Medical Subject Headings (MeSH)
Chemical synthesis

http://en.wikipedia.org/wiki/Aliskiren

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New Definition of MI Unveiled, Fractional Flow Reserve (FFR)CT for Tagging Ischemia

Posted in Bio Instrumentation in Experimental Life Sciences Research, Biomarkers & Medical Diagnostics, CABG, Cell Biology, Signaling & Cell Circuits, Chemical Biology and its relations to Metabolic Disease, Disease Biology, Small Molecules in Development of Therapeutic Drugs, FDA Regulatory Affairs, Frontiers in Cardiology and Cardiovascular Disorders, Health Economics and Outcomes Research, HealthCare IT, HTN, International Global Work in Pharmaceutical, Medical and Population Genetics, Medical Devices R&D Investment, Origins of Cardiovascular Disease, Personalized and Precision Medicine & Genomic Research, Pharmaceutical Industry Competitive Intelligence, Pharmacotherapy of Cardiovascular Disease, Population Health Management, Genetics & Pharmaceutical, Regulated Clinical Trials: Design, Methods, Components and IRB related issues, Technology Transfer: Biotech and Pharmaceutical, tagged American College of Cardiology, CABG, Conventional PCI, Coronary artery bypass surgery, Fractional Flow Reserve, Fractional Flow Reserve (FFR), Fractional Flow Reserve (FFR)CT, Journal of the American College of Cardiology, Kai Pharmaceuticals, OrbusNeich, PCI, Regado Biosciences, Roche Diagnostics, Seoul National University, St. Jude Medical on August 27, 2012| 19 Comments »

Reporter: Aviva Lev-Ari, PhD, RN

Updated 3/10/2013

Since August 25, 2012, when the ESC: New Definition of MI Unveiled was reviewed by Robert Jasmer, MD; Associate Clinical Professor of Medicine, University of California, San Francisco as was reported By Chris Kaiser, Cardiology Editor, MedPage Today, a new discussion emerged by ACC asking if FFR CT is Ready for prime time or not?

By Lisa Fratt

Mar 09, 2013

SAN FRANCISCO—Is there a better way to measure fractional flow reserve (FFR), Bon-Kwon Koo, MD, of Seoul National University queried a crowded room March 9 during an educational session at the American College of Cardiology (ACC) scientific session.

The current model is good for patients, safe and effective, Koo said. However, it requires an invasive procedure and is expensive. FFR _CT may provide a method to measure FFR without an invasive procedure.

FFR_CTextracts geometry from a CT scan to determine boundary conditions and fluid properties. In addition, velocity and pressure can be calculated. The hitch is that a supercomputer is required to solve the blood flow equation, said Koo. The results provide anatomical and functional data, thus giving a possible answer to the question at hand.

FFR_CTmay change daily practice in several ways. Most importantly, it may be a novel, fast, risk-free, noninvasive cost-saving way to measure FFR and identify patients who may not need to be sent to the cath lab for stenting or PCI. It can provide information to help surgeons plan strategies before invasive procedures, bypass procedures or interventional procedures. Noninvasive CT-derived FFR also can predict the functional significance of coronary lesions.

Despite its promise, however, FFR _CTis not ready for prime time, Koo said. FFR _CTdepends on the diagnostic accuracy of coronary CT angiography stenosis, which is less than true stenosis. With current technologies, true stenosis provides the required diagnostic accuracy.

FFR_CTis promising, but further development of the technology is required, Koo concluded.

http://www.cardiovascularbusiness.com/topics/imaging/acc-ffrct—ready-prime-time-or-not

ESC: New Definition of MI Unveiled

By Chris Kaiser, Cardiology Editor, MedPage Today

Published: August 25, 2012

Reviewed by Robert Jasmer, MD; Associate Clinical Professor of Medicine, University of California, San Francisco

MUNICH — An international, multispecialty task force has published a new definition of myocardial infarction that was prompted by the new generation of highly sensitive cardiac troponin (cTn) assays.

The highly sensitive assays are capable of detecting cTn in conditions other than MI, such as pulmonary embolism, cardiomyopathy, and left bundle branch block, and so result in false positives, according to the task force writing group.

The expert consensus document dips into a controversial area by setting levels of cTn for MI associated with percutaneous coronary intervention (PCI) and coronary artery bypass grafting (CABG).

“This is one of the most controversial areas in the definition of myocardial infarction,” Anthony DeMaria, MD, from the University of California in San Diego and editor-in-chief of the Journal of the American College of Cardiology, told MedPage Today.

“There are a large number of people undergoing PCI in the setting of an acute MI. It’s almost impossible to know whether a subsequent increase in troponin was part and parcel of the acute MI or related to the procedure itself,” DeMaria said.

The consensus document, titled “Third Universal Definition of Myocardial Infarction,” set the cTn levels for MI associated with PCI as elevation of troponin greater than 5 times the 99th percentile upper reference limit (URL) in patients with normal baseline levels or a rise in troponin values greater than 20% if the baseline values are elevated and are stable or falling.

“Some people speculate that troponin may be too sensitive in this situation and what is needed is evidence that an elevation of some degree of troponin following a procedure actually results in some alteration of the natural history of the patient,” DeMaria said. “In other words, the definition of acute MI after a procedure really is of significance if it increases the risk of subsequent events such as death.”

In CABG, the task force set the troponin values as greater than 10 x 99th percentile URL during the first 48 hours when baseline values are normal.

DeMaria said there are several ongoing studies examining the correlation of elevated cTn with subsequent events. As this is the third definition of MI since 2000, there most likely will be more refinements as new data emerge, he said.

The document is being copublished online in several journals including the Journal of the American College of Cardiology, Circulation, the European Heart Journal, and Global Heart.

The task force was in touch with the FDA during the development of this new definition, which means it could be used as the basis for clinical trial protocols designed according to FDA regulations.

“A universal definition for MI is of great benefit for clinical studies, since it will allow a standardized approach for interpretation and comparison across different trials,” the task force writing group explained.

When different definitions have been used in trials, it hampers “comparison and generalization between these trials,” they said.

Also of significance in this document is the inclusion of imaging as a means to identify or confirm an MI. The document spells out the strengths of echocardiography, nuclear imaging, MRI, and CT in the setting of acute MI.

“Imaging is playing an increasingly important role,” DeMaria said. “In the absence of focal symptoms or with an inconclusive ECG, it’s important to recognize the concomitant potential of ancillary measures, primarily imaging, to help with the diagnosis of a myocardial infarction.”

Thygesen reported relationships with Edwards Lifesciences, Servier, St. Jude Medical, Roche Pharma, and Roche Diagnostics. Her co-authors and reviewers reported relationships with Bayer Healthcare, Daiichi Sankyo, Johnson & Johnson, sanofi aventis, Servier, Novartis, Boehringer-Ingelheim, Genzyme, Eli Lilly, OrthoClinical Diagnostics, Abbott Laboratories, Alere, Brahms, Siemens Healthcare, Roche Pharma, Radiometer, BioRad, Diagenics, Response Medical, Takeda Pharmaceuticals, Regado Biosciences, Bristol-Myers Squibb, Merck Sharp and Dohme, GlaxoSmithKline, Merck, Portola Pharmaceuticals, AstraZeneca, Regado Biosciences, Scios, Ortho-Biotech, Pfizer, Kai Pharmaceuticals, Iroko Cardio, Philips, GE Healthcare, Boston Scientific, Lantheus, Medtronic, St. Jude Medical, Biotronik, Impulse Dynamics, Edwards Lifesciences, Health System Networks, Health Station Networks, Insight Telehealth Systems, Elsevier Sciences, Gilead, Evolva, Medicines Company, F. Hoffman La Roche, Torrent, Vifor International, Corthera, Nanosphere, Bayer Schering Pharma, Cardiorentis, Molecular Insight Pharmaceuticals, Berlin Chemie, Menarini, Cordis, Beckman Coulter, Amgen, Critical Diagnostics, Tethys Bioscience, Roche Diagnostics, bioMérieux, Genentech, Ikaria, Singulex, BG Medicine, Shionogi, Amylin, DiaDexus, Orion, WebMD, theheart.org, Pozen, Maquet, BHFZ, Covidien, Rapidscan, Actelion, Athera, Symetis, Schering-Plough, OrbusNeich, Terumo, Cardio3 Biosciences, Micell, Ablynx, Therabel, Kowa, Zentiva, Chugai Pharma, Automedics Medical Systems, Essentialis, Biosensors, Vascular Solutions, Zoll Medical, JaBA Recordati, Actavis, PharmaSwiss, Eisai, Medscape, Accumetrics, Bial Portela, AGA, Novo-Nordisk, Janssen-Cilag, Valtech, Otsuka Pharmaceuticals, Meda Pharma, CEPHALON, Intracellular Therapies USA, Santhera, TROPHOS, Pierre-Fabre, and Lundbeck.

DeMaria reported relationships with Gilead, ResMed Foundation, Lantheus, Cardiovascular Biotherapeutics, Angioblast Systems, General Electric Medical Systems, and Cardionet.

Primary source: European Heart Journal

Source reference:
Thygesen K, et al “Third universal definition of myocardial infarction” Eur Heart J 2012; DOI: 10.1093/eurheartj/ehs184.

http://www.medpagetoday.com/MeetingCoverage/ESCCongress/34368?utm_content=&utm_medium=email&utm_campaign=DailyHeadlines&utm_source=WC&xid=NL_DHE_2012-08-27&eun=g99985d0r&userid=99985&email=avivalev-ari@alum.berkeley.edu&mu_id=5099207

ESC: FFR CT Has Potential for Tagging Ischemia

By Chris Kaiser, Cardiology Editor, MedPage Today

Published: August 26, 2012

Reviewed by Robert Jasmer, MD; Associate Clinical Professor of Medicine, University of California, San Francisco

MUNICH — Using CT imaging to assess the hemodynamic significance of coronary lesions is “promising” but needs more research before it displaces conventional invasive fractional flow reserve (FFR), researchers said.

Using FFR as the reference standard, FFR_CTplus CT angiography (CTA) had good sensitivity (90%) and negative predictive value (84%) on a per patient basis for detecting ischemia, which indicates a low rate of false-negative studies, according to James K. Min, MD, of Cedars-Sinai Heart Institute in Los Angeles, and colleagues.

Although FFR_CT plus CTA were superior to CTA alone, the specificity (54%) and negative predictive value (67%) of the combination remained low compared with conventional FFR, indicating that a considerable number of false-positive studies would endure, Min reported here during a Hot-Line session at the European Society of Cardiology meeting.

The results of this proof of concept study show that FFR_CT can “impart considerable discriminatory power” to detect and exclude ischemia in patients with suspected CAD, Min said.

However, future studies should be conducted to determine the cost-effectiveness of FFR_CT in guiding decisions to stent, particularly given the potentially high false-positive rate, he added.

“Non-invasive FFR is a dream for all interventional cardiologists,” said study discussant Jean-Pierre Bassand, MD, of the University Hospital Jean-Minjoz in Besançon, France. Although Bassand praised the DeFACTO study, he expressed concern about the discrepancy between the accuracy of FFR versus FFRCT.

For example, compared with FFR, the sensitivity and specificity of FFRCT in cases of greater than 90% or less than 30% stenosis were 83% and 76%, respectively. The per-vessel correlation of FFRCT to FFR was 0.63.

“What matters is the correlation with FFR,” he concluded.

A single non-invasive imaging test that can identify obstructive coronary artery disease (CAD) and determine the physiological significance of those lesions would be ideal. At present, nuclear stress imaging fulfills the first part, but it cannot label stenoses as hemodynamically significant or not. Also, nuclear stress testing suffers from high rates of both false-negative and false-positive studies, Min said.

The results of this study are in line with stress imaging: per patient diagnostic accuracy of 73% (95% CI 67% to 78%). Min said that studies are being designed to compare FFR_CT plus CTA with stress imaging.

“For patients considered for invasive therapy, this type of test could help exclude those who don’t need to be stented,” Spencer King III, MD, of St. Joseph’s Hospital in Atlanta told MedPage Today.

“The excitement about this CT approach is that it moves things closer to being able to assess physiology and anatomy in a single non-invasive test,” added King, who is also a past president of the American College of Cardiology.

However, the process of calculating the FFR values from CT data currently takes about 6 hours, Min told MedPage Today. The CT data are sent offsite to HeartFlow, the company that makes the software. Whether such processing would be done onsite in the future is not yet determined, Min said. He also expects the processing time to drop to about 2 hours by the year’s end.

HeartFlow has already received EU mark to use the software in Europe and is in the process of applying for FDA approval, Min said.

Conventional FFR uses a pressure wire inserted through the groin to the coronary arteries to determine the hemodynamic significance of lesions. The same data can be gleaned during a typical CTA exam with software that calculates computational fluid dynamics,without additional radiation exposure. The median radiation exposure among the study centers was 6.4 mSv (range 4.4 to 15 mSv).

The original FAME study found the use of FFR to guide stenting was better than relying on angiography alone in patients with multivessel disease. A second study, FAME II, was stopped early because of the overwhelming benefit seen in patients with stable CAD when FFR guided stenting versus patients randomized to optimal medical therapy.

Because FFR_CT is a novel technique, it has not been adequately evaluated in its ability to identify patients with ischemia, Min said.

The researchers therefore designed the DeFACTO (Determination of Fractional Flow Reserve by Anatomic Computed Tomographic Angiography) study, which sought to evaluate the accuracy of FFR_CT while using invasive FFR as the reference standard.

The study was also simultaneously published online in the Journal of the American Medical Association.

The 252 patients with suspected or known CAD were recruited from 17 centers in five countries between October 2010 and October 2011. They were scheduled to undergo diagnostic catheter angiography.

The mean age of patients was 63, 70% were men, and a majority were white. Nearly half of the patients had obstructive CAD (>50% stenosis).

Among 615 study vessels, 271 had less than 30% stenosis and 101 had at least 90% stenosis. Invasive coronary angiography and FFR identified 46.5% of 408 vessels with obstructive CAD, while CT and FFR_CT identified 52.3% of 406 vessels.

A total of 172 patients had an FFR value <0.80, which indicates an ischemic lesion.

The diagnostic accuracy of FFR_CT plus CT was 73% (95% CI 67% to 78%), but this did not meet the prespecified primary endpoint of greater than 70% of the lower bound of the 95% confidence interval, Min said.

However, Min emphasized that FFR_CT was superior to CTA alone in all categories.

The researchers concluded that the results show the potential of FFR_CT as a “promising” non-invasive tool to identify ischemia.

King added that despite not meeting the prespecified primary endpoint, “it’s an encouraging early study.”

This study was funded by HeartFlow

Min reported relationships with GE Healthcare and Philips Medical. Some of his co-authors reported relationships with GE Healthcare, Siemens Medical Systems, Lantheus Medical Imaging, Boston Scientific, Merck, Abbott Vascular, Medtronic, Cordis, Eli Lilly, Daiichi Sankyo, Bristol-Myers Squibb, and sanofi-aventis.

King reporeted relationships with Merck & Company, Wyeth Pharmaceuticals, Celonova Biosciences, and Northpoint Domain.

Primary source: Journal of the American Medical Association
Source reference:
Min J, et al “Diagnostic accuracy of fractional flow reserve from anatomic CT angiography” JAMA 2012; DOI: 10.1001/2012.jama.11274.

Additional source: Journal of the American Medical Association
Source reference:
Patel, MR et al “Detecting obstructive coronary disease with CT angiography and noninvasive fractional flow reserve” JAMA 2012; DOI: 10.1001/2012.jama.11383.

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Age-Dependent Depression in Circulating Endothelial Progenitor Cells in Coronary Artery Bypass Grafting Patients

Posted in CABG, Cardiac & Vascular Repair Tools Subsegment, Cardiovascular Pharmacogenomics, Pharmacotherapy of Cardiovascular Disease, Population Health Management, Genetics & Pharmaceutical, tagged Age, Cardiac surgery, Cardiovascular disease, Cardiovascular Disorders, Coronary Artery Bypass Grafting, endothelial progenitor cells on August 17, 2012| 2 Comments »

Reporter and Curator: Dr. Sudipta Saha, Ph.D.

Coronary artery bypass grafting (CABG) or percutaneous transluminal coronary angioplasty (PTCA) is used to reconstitute flow into post-stenotic, chronically underperfused myocardium. This post-stenotic myocardium consists of connective tissue scars, dying cardiomyocytes, and hypo-active or chronically hibernating myocardium with microvascular disturbances due to microthrombi and decreased capillary density. When bulk flow is successfully reconstituted by CABG or PTCA, the gradual recovery of microcirculation is considered as decisive for the recovery of mechanical function of surviving post-stenotic myocardium. Traditionally, neovascularization of disturbed microcirculation was considered to result exclusively from the proliferation, migration, and remodeling of fully differentiated endothelial cells (ECs) derived from pre-existing blood vessels. Recently, however, it was demonstrated that circulating, bone marrow-derived endothelial progenitor cells (EPCs) may home to sites of postnatal neovascularization and differentiate into ECs in situ, which is called “vasculogenesis”. Vascular trauma, as it occurs during surgical procedures, or inflammation leads to a cascade of events that result in the chemoattraction of inflammatory cells or other cell types to the site of injury. These blood-borne cells produce pro-angiogenic factors that, in turn, attract other cell types such as circulating EPCs. Systemic inflammatory responses have been described after cardiac surgery with cardiopulmonary bypass (CPB). Contact of the blood components with the artificial surface of the extracorporeal circuit, ischemia-reperfusion injury, endotoxemia, and operative trauma are possible causes for this phenomenon. Trauma has been considered as the critical stimulus for the mobilization of EPCs and proangiogenic vascular endothelial growth factor (VEGF) during CABG. It has been speculated that this mobilization may contribute to the revascularization of injured tissue, which would be of great clinical relevance for a successful outcome of CABG. Presently, there is a strong trend to perform CABG in patients of advanced age. However, experimental data indicate impaired neoangiogenesis in ischemic tissues and impaired re-endothelialization of vascular lesions as a function of advanced age. The mechanisms for this age-dependent impairment of vascular repair are largely unknown. Therefore, we analyzed the influence of age on CABG-induced mobilization of EPCs and cytochemokines with angiogenesis-modulating potential in a cohort of consecutive patients with stable coronary artery disease (CAD) scheduled for elective CABG. Probably, several types of endothelial precursor or progenitor cells have angiogenic potential after homing into traumatic tissue. Therefore, we used two phenotypic markers (CD34 and AC133 or CD133), which are expressed in all EPC types, but in the case of AC133, not in differentiated ECs. This was done to exclude from our analysis any mature or dying ECs with doubtful angiogenic capacity, potentially released from damaged vessels in old patients. In this analysis, we demonstrate that the preoperative number of circulating EPCs in patients with stable CAD is reduced with increasing age, together with decreased plasma VEGF levels. During CABG, mobilization of circulating EPCs could be detected in all patients, but this mobilization remained on a persistently lower level in the older patient group, suggesting that the responsiveness for mobilization of EPCs is impaired with age. Optimized strategies for ex-vivo expansion of those cells might be especially required in the elderly, if transplantation of these cells into poststenotic tissue will develop as a future co-therapy to existing interventions of revascularization.

This study demonstrated that the basal number of circulating EPCs in patients with stable CAD is decreased with increasing age. Furthermore, plasma VEGF levels are reduced with increasing age. This age-associated decrease could not be explained by higher prevalences of other risk factors, such as male gender, diabetes mellitus, hypertension, or hyperlipoproteinemia at older ages nor by any differences in left ventricular function or New York Heart Association classes. The operative trauma of complex cardiac surgery with CPB induced a mobilization in EPCs/ lymphocytes and EPCs/blood in all patients, but this mobilization remained on a persistently lower level in the older patient group, which could not be explained by any differences in the operative procedure (time on CPB, cross-clamping time, or number of grafts) or in the operation-induced increase in cytochemokines with a reported potency for modulation of angiogenesis (IL-6, IL-8, and IL-10). Similar age-associated losses in the number of circulating endothelial-related progenitor cells in patients undergoing CABG have not been reported so far. In 45 male subjects without a history of cardiovascular disease, the Framingham risk score and impairment of endothelium-mediated, flow-dependent brachial artery dilation were strong predictors of depressed numbers in circulating progenitor cells with colony-forming capacity. In a mixed group of healthy probands and CAD patients, Vasa et al. reported age-associated losses in circulating cells positive for CD34_ and KDR_, which may include progenitor cells and mobilized ECs. In their cohort, smoking was a strong predictor of lowered values in CD34_/KDR_ cells, independent of age. In the patients, self-reported smoking status, which is notoriously unreliable before cardiac surgery, could not be verified by interrogations of spouses or relatives. This may explain why we could not detect an effect of smoking on circulating EPCs. The reasons for the age-associated losses in circulating EPCs remain unknown at present. In this study, there was an age-independent correlation of circulating EPCs with plasma VEGF levels. Circulating or transplanted EPCs contribute to post-ischemic neovascularization in animal experiments and patients, and angiogenic factors like VEGF and PlGF are involved in this neovascularization. In animals, advanced age is associated with attenuated post-ischemic neovascularization and attenuated local induction of VEGF. Similarly, arterial re-endothelialization after vascular trauma is attenuated in old animals in which trauma-induced local VEGF expression is lower and local VEGF supplementation rescues vascular healing. Experimental elevation of plasma VEGF in mice by inoculation with adenoviral vectors induced rapid mobilization of endothelial precursor cells. Therefore, it is tempting to propose that lowered VEGF levels in the elderly patients are the reason for lowered circulating EPCs. However, this causality remains to be proven for basal steady-state levels, and the cause of depressed circulating VEGF levels in elderly patients remains unknown. In experimental studies, hypoxia-inducible factor-1 stabilization by hypoxia, which mediates hypoxic VEGF expression, is attenuated in cells from old animals. This might be relevant for the attenuated and retarded CABG-induced activation of plasma VEGF in older patients. However, this may be less relevant for the age-associated lowering in basal VEGF levels before surgery. Local and systemic inflammation by vascular trauma is considered an important contributor of post-ischemic neovascularization. In the patients, the operative trauma resulted in a substantial mobilization of cytochemokines with angiogenesis-modulating potential, except for IL-18 and PlGF. These observations are in agreement with previous reports. Although none of these activated factors could be directly correlated with the individual increase in EPCs during and after the operation in the patients, it is reasonable to assume that the complex spectrum of inflammatory activation is contributing to the mobilization of surgery-induced EPCs. Similar conclusions have been derived from observations on transient mobilization of KDR_/AC133_ cells in patients after burns or CABG. The kinetics of mobilization in that study differed somewhat from our observations, but the two studies are not directly comparable owing to differences in progenitor cell analysis. It is remarkable that the substantial inflammatory activation during surgery in our study could not abolish age-associated differences in EPC levels. The decline in the fraction of lymphocytes/leukocytes after CPB down to one-quarter that of the baseline value at 12 h after CPB most likely reflects substantial homing of lymphocytes into tissues in response to the systemic inflammatory activation induced by CPB. Homing must also contribute to the decline of circulating EPCs/ blood during this time. Therefore, circulating EPC levels underestimate the amount of EPC mobilization. However, quantification of lymphocyte or EPC homing could not be obtained in our patients. Application of different populations of EPCs or other mononuclear bone marrow cells improves postischemic organ function and microcirculation in animals and patients. However, it is not clear whether the surgery-induced mobilization of EPCs is sufficient for such a contribution. Furthermore, it is unclear whether the EPCs in elderly patients have the same angiogenic potential compared with those of younger patients. The EPCs collected from the circulation can be amplified in vitro. The co-application of amplified EPCs, together with native artery recanalization or bypass grafting, probably will develop as a therapeutic option in the future. The experimental data suggested that such co-therapy is especially desirable in elderly patients. The data suggested that mobilization of such cells for therapeutic application might be more difficult with an increasing age of patients. The inflammatory activation by complex CABG does not offset this age-associated lowering. Therefore, further studies are required for a better understanding of optimized strategies for recruitment, ex-vivo expansion, and retransplantation strategies involving EPCs in aging patients.

Abbreviations and Acronyms:

APC _ allophycocyanin

CABG _ coronary artery bypass grafting

CAD _ coronary artery disease

CPB _ cardiopulmonary bypass

EC _ endothelial cell

EPC _ endothelial progenitor cell

KDR _ kinase insert domain containing receptor

IL _ interleukin

PlGF _ placental growth factor

PTCA _ percutaneous transluminal coronary angioplasty

VEGF _ vascular endothelial growth factor

Source reference:

http://www.sciencedirect.com/science/article/pii/S0735109703012725

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Competition in the Ecosystem of Medical Devices in Cardiac and Vascular Repair: Heart Valves, Stents, Catheterization Tools and Kits for Open Heart and Minimally Invasive Surgery (MIS)

Posted in Aortic Valve: TAVR, TAVI vs Open Heart Surgery, Bio Instrumentation in Experimental Life Sciences Research, CABG, Cardiac & Vascular Repair Tools Subsegment, Ecosystems & Industrial Concentration in the Medical Device Sector, Frontiers in Cardiology and Cardiovascular Disorders, Massachusetts Niche Suppliers and National Leaders, Medical Devices R&D and Inventions, Medical Devices R&D Investment, Mitral Valve: Repair and Replacement, Pharmacotherapy of Cardiovascular Disease, Stents & Tools, Valves & Tools, tagged Angioplasty Suite, Cardiac & Vascular Repair, Cardiac Surgery Operating Room, Industry Concentration Ratio in Medical Devices Markets, Market Penetration Cost, Market Penetration in Medical Devices Market, National Leader Supplier, Niche supplier, Potential Revenue by Partnership Options on June 22, 2012| 20 Comments »

Competition in the Ecosystem of Medical Devices in Cardiac and Vascular Repair: Heart Valves, Stents, Catheterization Tools and Kits for Open Heart and Minimally Invasive Surgery (MIS)

Curator: Aviva Lev-Ari, PhD, RN

This report covers the following product categories

Heart Valve Frames:

Transcatheter Aortic-Valve Implantation (TAVI) and Replacement (TAVR)
Aortic-Valve Implantation and Replacement in Open Heart Surgery (AVR)
Mitral Valve

Stents:

Coronary stents
Neurovascular stents
Carotid stents
Peripheral stents
Biliary stents

Surgical tools:

Endoscopic surgical tools
Guide wires for trans-catheter interventions (angioplasty)

The National Leader Supplier Edwards Lifesciences and its SAPIEN product for Transcatheter Aortic-Valve Implantation (TAVI) and Replacement (TAVR) is covered in Executive Compensation and Comparator Group Definition in the Cardiac and Vascular Medical Devices Sector: A Bright Future for Edwards Lifesciences Corporation in the Transcatheter Heart Valve Replacement Market 6/20/2012

http://pharmaceuticalintelligence.com/2012/06/19/executive-compensation-and-comparator-group-definition-in-the-cardiac-and-vascular-medical-devices-sector-a-bright-future-for-edwards-lifesciences-corporation-in-the-transcatheter-heart-valve-replace/

The ecosystem of Cardiac and Vascular Surgery for Repair or Replacement by Implantation of a new blood vessel or medical device covers the following procedure-related devices and tools now in use:

Arterial catheterization kit
Embolectomy catheters
Occlusion catheter
Coronary stents
Neurovascular stents
Carotid stents
External and internal carotid shunts
Peripheral stents
Biliary stents
Micro vascular clips
Stainless steel tunneler vascular graft
Cardiopulmonary bypass vascular catheter
Coronary stent graft system
Catheter tip occluder
Synthetic/biological composite vascular graft
Valvulotome tools
Aortic Valve
Mitral Valve
Angioplasty Guided Wires

Product Category Total US and Total Global Suppliers, Suppliers in MA by Product, Segment Industry Concentration in the US and in MA

Cardiology & Vascular Surgery Tools and Devices in use	Total number of Suppliers	GlobalSupplier	US Supplier	Suppliers in Massachusetts	Segment ConcentrationRatio in US Market	Segment Concentration Ratio in the State of MA
Arterial catheterization kit	10[MA=2]	4	6	Lemaitre Vascular, Inc. www.lemaitre.comBurlington Smiths Medical ASD, Inc Weston	5.6	3.6
Embolectomy catheters	39[MA=3]	11	28	Lemaitre Vascular, Inc. www.lemaitre.comBurlington Clinical Instruments Intl., Inc. Southbridge Boston Scientific Corporation www.bostonscientific.com Natick	1.9	2.4
Occlusion catheter	8[MA=3]	1	7	Lemaitre Vascular, Inc. www.lemaitre.comBurlington Boston Scientific Corporation www.bostonscientific.com Natick Telemed Systems Inc. www.telemedsystems.com Hudson	2.8	2.4
Coronary stents	45[MA=2]	11	34	Lemaitre Vascular, Inc. www.lemaitre.comBurlington Boston Scientific Corporation www.bostonscientific.com Natick	1.7	2.6
Neurovascular stents	8[MA=1]	2	6	Boston Scientific Corporation www.bostonscientific.comNatick	4.5	5.5
Carotid stents	13[MA=1]	1	12	Boston Scientific Corporation www.bostonscientific.comNatick	1.7	5.5
External and internal carotid shunts	7[MA=2]	2	5	Bard Electrophysiology www.bardep.comLowell Lemaitre Vascular, Inc. www.lemaitre.com Burlington	5.5	3.7
Peripheral stents	7[MA=1]	0	7	Boston Scientific Corporation www.bostonscientific.comNatick	1.0	1.0
Biliary stents	20[MA=1]	7	13	Boston Scientific Corporation www.bostonscientific.comNatick	3.1	3.6
Micro vascular clips	9[MA=2]	3	6	Lemaitre Vascular, Inc. www.lemaitre.comBurlington Life Instrument Corporation www.lifeinstruments.com Braintree	5.2	3.7
Stainless steel tunneler vascular graft	6[MA=1]	3	3	Lemaitre Vascular, Inc. www.lemaitre.comBurlington	10.0	5.1
Cardiopulmonary bypass vascular catheter	53[MA=5]	14	39	Abiomed, Inc. www.abiomed.comDanvers Vortex Medical Inc www.angiovac.com Norwell Lemaitre Vascular, Inc. www.lemaitre.com Burlington Clinical Instruments Intl., Inc. Southbridge Smiths Medical ASD, Inc Weston	1.6	2.0
Coronary stent graft system	6[MA=1]	0	6	Lemaitre Vascular, Inc. www.lemaitre.comBurlington	1.0	1.0
Catheter tip occluder	7[MA=2]	1	6	Lemaitre Vascular, Inc. www.lemaitre.comBurlington Clinical Instruments Intl., Inc. Southbridge	3.3	3.3
Synthetic/biological composite vascular graft	8[MA=2]	3	5	Lemaitre Vascular, Inc. www.lemaitre.comBurlington Boston Scientific Corporation www.bostonscientific.com Natick	6.3	3.7
Valvulotome tools	9[MA=1]	3	6	Lemaitre Vascular, Inc. www.lemaitre.comBurlington	5.2	5.1
Aortic Valve	11[MA=0]	2	9	none	2.9	10.0
Mitral Valve	11[MA=0]	4	7	none	4.8	6.4
Angioplasty Guided Wires	21[MA=2]	8	11	Arrow International, Walrus DivisionWoburn Boston Scientific Corporation www.bostonscientific.com Natick	3.7	3.0

Source: Name of products and Names of Suppliers were extracted from: http://www.medicregister.com/Cardiology_Vascular_Surgery/Categories/cid2.htm

Industry Segment Concentration Ratio: Impact on Market Penetration Cost and Potential Revenue and Market Share per Product Line

Industry Concentration Ratios per Product Line in the Cardiac and Vascular Medical Devices Segments
A	B	C	D	E	F	G	H	I	J
		US comparison				MA comparison
Cardiology & Vascular Surgery Tools and Devices in use	Global Suppliers	US Suppliers	Market share	Global ratio	Index	MA Suppliers	Market share	Global ratio	Index
Arterial catheterization kit	4	6	0.09	0.40	5.6	2	0.14	0.67	3.6
Embolectomy catheters	11	28	0.03	0.28	1.9	3	0.07	0.79	2.4
Occlusion catheter	1	7	0.11	0.13	2.8	3	0.20	0.25	2.4
Coronary stents	11	34	0.02	0.24	1.7	2	0.07	0.85	2.6
Neurovascular stents	2	6	0.11	0.25	4.5	1	0.25	0.67	5.5
Carotid stents	1	12	0.07	0.08	1.7	1	0.33	0.50	5.5
External and internal carotid shunts	2	5	0.13	0.29	5.5	2	0.20	0.50	3.7
Peripheral stents	0	7	0.13	0.00	1.0	1	0.50	0.00	1.0
Biliary stents	7	13	0.05	0.35	3.1	1	0.11	0.88	3.6
Micro vascular clips	3	6	0.10	0.33	5.2	2	0.17	0.60	3.7
Stainless steel tunneler vascular graft	3	3	0.14	0.50	10.0	1	0.20	0.75	5.1
Cardiopulmonary bypass vascular catheter	14	39	0.02	0.26	1.6	5	0.05	0.74	2.0
Coronary stent graft system	0	6	0.14	0.00	1.0	1	0.50	0.00	1.0
Catheter tip occluder	1	6	0.13	0.14	3.3	2	0.25	0.33	3.3
Synthetic/biological composite vascular graft	3	5	0.11	0.38	6.3	2	0.17	0.60	3.7
Valvulotome tools	3	6	0.10	0.33	5.2	1	0.20	0.75	5.1
Aortic Valve	2	9	0.08	0.18	2.9	0	0.33	1.00	10.0
Mitral Valve	4	7	0.08	0.36	4.8	0	0.20	1.00	6.4
Angioplasty Guided Wires	8	11	0.05	0.42	3.7	2	0.09	0.80	3.0
					126				27
Source for A, B, C, G – http://www.medicregister.com
Source for D,E,F,H,I,J -Computed ratios per formulas below by Aviva Lev-Ari, PhD, RN
D = 1/(1+B+C) = projected market share assuming non-differential production capacity

E = B/(B+C) = fraction of global among all suppliers

F = DE$F$24+1 = product of “D” and “E”, scaled to be in the range from 1 to 10

“H” is the same as “D” but with MA suppliers replacing “US suppliers”
“I” is the same as “E” but with MA suppliers replacing “US suppliers”
“J” is the same as “F” but with MA suppliers replacing “US suppliers”

Penetration Strategy for a Global Supplier Targeting the US Market and the Massachusetts Market

Customized predictions of penetration cost and estimation of potential revenues based on the industry segment concentration ratios in the Table above are part of an Actionable Strategic Market Entry Plan into the US market.

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National Medical Device Suppliers within the Cardiac and Vascular Repair Market by Product Category

Cardiology vascular surgery – The OR equipment

Bard Electrophysiology www.bardep.com

Lowell, Massachusetts Bard Electrophysiology develops & markets products, which aid in the diagnosis and treatment of electrophysiology disorders. Our products include therapeutic, diagnostic & mapping, intracardiac access, temporary pacing electrodes, and EP systems. Our Scorpion®2 Ablation Catheter brings exception more…

Edwards Lifesciences Corporation www.edwards.com

Irvine, California Edwards Lifesciences Corporation delivers acute hemodynamic monitoring & heart valves. Our new perimount magna heart valve (bioprosthesis), with its supra-annular design, offers optimal hemodynamics and flow characteristics for treatment of aortic heart valve diseases. Our embolectomy catheters are more…

Bridgepoint Medical, Inc. www.bridgepointmedical.com

Plymouth, Minnesota Bridgepoint Medical, Inc. deals with the field of interventional cardiology for access to and treatment of chronic total occlusions(CTOs). The Crossboss™ CTO catheter and the Stingray™ CTO re-entry system are used to improve physician access to chronic total occlusions. This occlusion oc more…

Futurematrix Interventional +1-(903)-6779166

Athens, Texas Futurematrix Interventional supplies a range of disposable medical devices. Our products include catheters and stents, angioplasty & angiography catheters, vascular stent delivery systems, hydrophilic urethral stents, and biopsy guns. We provide radiology, cardiology, and urology applications. We al more…

Edwards Lifesciences Technology Sarl +1-(949)-250-2500

Anasco Edwards Lifesciences Technology Sarl offers surgical products. Our products include angiography catheters, arterial blood sampling kit, central venous catheter kit, disposable pressure dome, irrigation catheter, fluid delivery tubing, vascular clamps, physiological patient monitors, intravascular ad more…

Peridot Corporation www.peridotcorp.com

Pleasanton, California Peridot Corporation specializes in the production of medical products. We provide pulmonary drug delivery systems, cardiovascular & gastrointestinal treatments, rf/thermal ablations, laproscopic, endoscopic instruments, & arthroscopic instruments, chemotherapy & stent delivery systems and catheters. more…

Medtronic Ablation Frontiers LLC www.ablationfrontiers.com

Carlsbad, California Medtronic Ablation Frontiers LLC is specialized in the treatment of ablation therapy by developing safety devices & solutions for individuals suffering from atrial fibrillation & other cardiac arrhythmias. Our product, cardiac ablation per-cutaneous catheter provides a minimally invasive treatment f more…

Endophotonix, Inc +1-(651)-452-3000

Eagan, Minnesota Endophotonix Inc. designs and manufactures laser-based surgical ablation systems. The products are indicated for the delivery of laser light for the incision, excision, dissection, vaporization, ablation or coagulation of soft tissue, including cardiac tissue, during surgical procedures. The Atrilaz more…

Csa Medical, Inc. www.csamedical.com

Baltimore, Maryland Csa Medical, Inc. deals with cryospray ablation systems. Our cryospray ablation system removes diseased tissue by rapidly freezing and thus destroying the unwanted tissue. The system transports low-pressure liquid nitrogen through a specially designed catheter that is passed through a standard endos more…

Guidant Corporation www.guidant.com

St. Paul, Minnesota Guidant Corporation is involved in the design and development of cardiovascular medical products. We offer products for the treatment of arrhythmias, heart failure, coronary artery and peripheral vascular diseases. Our implantable cardioverter defibrillators are used to treat heart rhythms that are more…

Biotronik GmbH & Co. www.biotronik.com

Germany Biotronik GmbH & Co. manufactures medical products for the electrotherapy of the heart and vascular intervention. Our astron pulsar self-expanding stent utilises technology in stent conception to create a device that ensures flexibility & improved vessel wall scaffolding. Our Pheron® offers a le more…

Medtronic CryoCath LP www.cryocath.com

Quebec, Canada Medtronic CryoCath LP is a medical technology company that creates catheters & probe-based cryotherapy products to treat cardiovascular diseases. We offer products such as Freezor®, Freezor® Xtra, Freezor® MAX & CryoConsole. Our product medtronic cryocath has developed a minimally invasiv more…

Cardima, Inc. www.cardima.com

Fremont, California Cardima, Inc. designs, manufactures & markets microcatheter systems for the mapping & ablation of cardiac arrhythmias. Arrhythmias are abnormal electrical heart rhythms that adversely affect the mechanical activities of the heart and can significantly affect a person’s quality of life & be potential more…

Alsius Corporation www.alsius.com

Irvine, California Alsius Corporation specializes in intravascular thermal regulation technology. Our Icy™ catheter is inserted into the femoral vein and resides in the inferior vena cava. It delivers target temperature and control rewarm after cooling in neuro surgery & cardiac surgery. All Alsius® heat exc more…

Flowcardia, Inc. www.flowcardia.com

Sunnyvale, California Flowcardia, Inc. deals with the design and development of a portfolio of catheter-based technologies to facilitate guidewire crossing of totally occluded coronary & peripheral arteries. Our Crosser® 14 catheter uses high-frequency vibration to facilitate navigation of guidewires beyond chronic t more…

Venetec International, Inc. venetec.com

San Diego, California Venetec International, Inc. supplies medical products. We specialize in catheter securement technology. Our Statlock® devices protect patients and healthcare workers by reducing potential complications & accidental needlesticks. Our StatLock® stabilization devices replace tape & suture, redu more…

Codman & Shurtleff, Inc. www.codman.com

Raynham, Massachusetts Codman & Shurtleff, Inc. develops and markets a wide range of diagnostic & therapeutic products for the treatment of central nervous system disorders. Our focus is on intractable pain management, pediatric & adult hydrocephalus, and neuro critical care. Our product line includes drug pumps, cerebros more…Geister Medizintechnik GmbH www.geister.com

Tuttlingen, Germany Geister Medizintechnik GmbH is a manufacturer of specialized surgical products carrying a full range of advanced surgical instruments and devices. We work in the three business fields such as cardio, neuro and powered. We develop innovative product and process solutions for coronary artery bypass gr more…

Kaisers Surgical Instruments Pty Ltd www.kaisers.com.au

Western Australia, Australia Kaisers Surgical Instruments Pty Ltd is a supplier of high quality Kaiser branded surgical instruments. Our instrument menu comprises of orthopaedic, ophthalmic, general, ENT and cardio instruments. Our repair service offers a fast and efficient means of restoring damaged surgical instruments regard more…

Arterial catheterization kit suppliers

Arrow International, Inc. www.arrowintl.com

Reading, Pennsylvania Arrow International, Inc. combines technology and product innovation to extend the use of catheterization for the diagnosis & treatment of critically ill patients. Our disposable critical care catheterization products are used principally to access the central vascular system for administration of f more…

Lemaitre Vascular, Inc. www.lemaitre.com

Diablo Sales & Marketing, Inc. www.diablosales.com

Diablo, California Diablo Sales & Marketing, Inc. specializes in OEM components to the medical device and high technology sectors. We provide resources for new product designs incorporating the latest engineered material design technologies. We have access to CAD/CAM, solid works and pro/engineer technology for design more…

Angiodynamics, Inc. www.angiodynamics.com

Queensbury, New York Angiodynamics, Inc. provides medical devices for radiologists, surgeons, and other physicians. We offer medical devices for the minimally invasive diagnosis and treatment of cancer and peripheral vascular disease. Our product line includes market-leading radio frequency ablation systems, vascular ac more…

Smiths Medical ASD, Inc

Weston, Massachusetts Smiths Medical ASD, Inc supplies devices that are used during critical & intensive care, surgery, post-operative care during recovery & in a series of high-end home infusion therapies. We focus on developing technologies that offer both clinical & economic advantages to our healthcare providers and more…

Ayra Medikal Yatirimlar Limited Sirketi

Dikmen, Turkey Ayra Medikal Yatirimlar Limited Sirketi manufactures and distributes range of disposable medical devices for use in cardiology, radiology, critical care unit and operation rooms. more…

Intra Special Catheters GmbH www.intra-online.de

Germany Intra Special Catheters GmbH specilizes in catheters. Our product range comprises of arterial catheters, thoracic drainage catheters, central venous catheters and catheters for vessel surgery. The Microseld PTFE is suited for non-traumatic puncture of peripheral arteries for complication-free positi more…

Marconi Medizintechnik Deutschland GmbH +49-(6122)-9140

Germany Marconi Medizintechnik Deutschland GmbH offers medical products. more…

Biomedical Industry Group Inc. www.biomedgroup.com

Ontario, Canada Biomedical Industry Group Inc. manufactures Rollachair™, Needlegard™, Catheterdriver™ and Arterialpressurestand™. Our Rollachair™ is hygienic and meets infection control standards. Our pressure stand is used with a sterile pad during arterial catheterization process. more…

Embolectomy catheters suppliers

Arrow Internacional De Mexico, S.A. De C.V. +52-(610)-378-0131

Mexico Arrow Internacional De Mexico, S.A. De C.V. offers multiple sterile needleless injection hub, wire guides and various intravascular catheters. more…

Atrium Medical Corporation www.atriummed.com

Hudson, New Hampshire Atrium Medical Corporation manufactures breakthrough medical device technologies used in open heart surgery, emergency chest trauma, thoracic drainage and surgical repair of diseased blood vessels. We are an ISO 9000, ISO 9001, ISO 9002 & CE MARK certified company. We offer products like cardiology, more…

Ev3, Inc. www.ev3.net

Plymouth, Minnesota Ev3, Inc. is a medical device company that focuses on catheter based or endovascular, technologies for the minimally invasive treatment of vascular diseases and disorders. We offer neuro products such as embolic coils, liquid embolics, micro catheters, Guidewires, balloons, carotoid stents & embolic more…

Alsius Corporation www.alsius.com

Cook Vascular IncorporatedSEND INQUIRY

Vandergrift, Pennsylvania Cook Vascular Incorporated provides interventional, therapeutic and diagnostic vascular products. We also manufacture a complete line of Vital-port® vascular access ports and a wide variety of catheters, introducers & specialty components. Our lead extraction system is a collection of specialize more…

Vascular Solutions Inc. www.vascularsolutions.com

Minneapolis, Minnesota Vascular Solutions Inc. develops products for the interventional cardiologist and interventional radiologist. Our D-Stat products are based on the scientifically proven hemostatic power of thrombin. Our Vari-Lase endovenous laser system is designed to help physicians provide advanced treatment for v more…

Cook Group Incorporated www.cookgroup.com

Bloomington, Indiana Cook Group Incorporated focuses on the research and product development in minimally invasive medical device technology for diagnostic & therapeutic procedures. Our wire-guided arndt endobronchial blocker set allows one-lung ventilation using a conventional endotrachael tube and a pediatric fiberopt more…

Cordis Corp. +1-(786)-313-2000

Miami Lakes, Florida Cordis Corp., a Johnson & Johnson company develops products to treat circulatory system diseases including congestive heart failure and cerebral aneurysms. Its product lines include the balloons, catheters, forceps, guidewires, and plain and drug-coated stents used in cardiology, endovascular, and n more…

Edwards Lifesciences Corporation www.edwards.com

Medtronic Xomed Surgical Products, Inc www.xomed.com

Jacksonville, Florida Medtronic Xomed Surgical Products, Inc develops products that treat people with ear, nose and throat (ENT) diseases. our products include MeroPack®, Bioresorbable Nasal Dressing and Sinus Stent, Integrated Power Console System, Pillar® System, Big Easy® Piston, and ENT-5000 Video Endosco more…

Merit Medical Systems, Inc. www.merit.com

South Jordan, Utah Merit Medical Systems, Inc. manufactures medical devices used in diagnostic and interventional cardiology & radiology procedures. Our primary products are inflation devices, diagnostic and therapeutic catheters, guide wires, pressure monitoring disposables, fluid delivery systems, medication syringe more…

Medtronic, Inc. www.medtronic.com

Minneapolis, Minnesota Medtronic, Inc. specializes in medical technology, thus providing lifelong solutions for people with chronic pain. We focus on cardiac rhythm disease management (CRDM), spinal & biologics, cardiovascular, neuromodulation, diabetes, and surgical technologies. Our cardiac resynchronization therapy (CR more…

Hotspur Technologies, Inc. www.hotspur-inc.com

Mountain View, California Hotspur Technologies, Inc. develops catheter-based technologies aimed at restoring blood flow for patients with obstructed vessels. The IQCath™ balloon dilatation catheter is a specialty three-in-one device that allows the physician to perform angioplasty, deliver targeted contrast, and perfor more…

Nexgen Medical Systems, Inc.SEND INQUIRY

Reno, Nevada Nexgen Medical Systems, Inc. specializes in developing medical devices. Our medical devices improve safety & efficacy of interventional procedures in patients with neurological and cardiovascular diseases. Our products include embolic protection device, and mechanical clot retrieval device. We provi more…

Pfm Medical, Inc www.pfmmedical.com

Oceanside, California Pfm Medical, Inc specializes in products such as EZ Huber®, pfm PICC Catheters, and interventional cardiology. The EZ huber isolates the caregiver from harmful patient fluids and oncology drug splatter. PICC catheters & trays provides increased flexibility to both administer and medications & pe more…

Lemaitre Vascular, Inc. www.lemaitre.com

Micrus Endovascular Corporation www.micrusendovascular.com

San Jose, California Micrus Endovascular manufactures & markets both implantable and disposable medical devices used in the treatment of cerebral vascular diseases. Our products are used by interventional neuroradiologists and neurosurgeons primarily, to treat cerebral aneurysms in the brain which are responsible for he more…

Spectranetics Corporation, The www.spectranetics.com

Colorado Springs, Colorado The Spectranetics Corporation manufactures and markets the excimer laser system for use in minimally invasive interventional procedures within the cardiovascular system. The spectranetics laser system utilizes a wavelength of 308 nanometers in the ultraviolet region of the light spectrum. The laser more…

Artegraft, Inc. www.artegraft.com

North Brunswick, New Jersey Artegraft, Inc. specializes in offering Collagen Vascular Graft™. Artegraft is a natural collagen vascular graft. Its biological fibrous matrix is processed to enhance long term patency and provide a tightly woven, cross-linked conduit that is flexible & compliant. It is used for segmental byp more…

Arrow International, Inc www.neocare.com

San Antonio, Texas Arrow International, Inc. develops, manufactures and markets a broad range of catheter based therapeutic products. Our Arrow SmartSeal™ hemostatic peelable dialysis sheath is designed to minimize risk of air embolism, minimize blood loss, and reduce clinician’s exposure to blood-borne pathogen more…

Lumen Biomedical, Inc. www.lumenbio.com

Plymouth, Minnesota Lumen Biomedical, Inc. offers interventional devices for embolic protection and thrombus removal throughout the body. Our FiberNet® embolic protection system features a low crossing profile for optimal device deliverability. Its proprietary filter design promotes conformability to asymmetrical v more…

Lucas Medical, Inc. www.lucasmedicalinc.com

Anaheim, California Lucas Medical, Inc. specializes in silicone medical products. Our product portfolio comprises of embolectomy catheters, occlusion catheters, biliary catheters, carotid shunts, thrombectomy catheters, straight irrigation catheters and bi-lumen irrigation catheters. Our arterial embolectomy catheters more…

Clinical Instruments Intl., Inc. +1-(508)-764-2200

Southbridge, Massachusetts Clinical Instruments Intl., Inc. provides carotid bypass shunt, introducers and detergent reagent. more…

Biosensors International USA www.biosensors.com/usa

Newport Beach, California Biosensors International USA develops, manufactures and markets medical devices for interventional cardiology & critical care procedures. Acutrans™ is our fully disposable blood pressure transducer system that is used in invasive blood pressure measurement with lowest possibility of zero drift more…

Applied Medical www.appliedmedical.com

Rancho Santa Margarita, California Applied Medical is associated with clinical areas such as general surgery, urology, vascular, cardiac, colorectal and Ob/Gyn surgery. We have introduced GelPort® laparoscopic system, Kii® abdominal access system, Acucise® endopyelotomy/endoureterotomy system, Direct Drive® graspers a more…

Sorin Group USA, Inc. www.soringroup-usa.com

Arvada, Colorado Sorin Group USA, Inc. designs and manufactures cardiac perfusion & blood management systems. Our D100 oxygenator is designed for neonatal procedures. It is designed to reduce allogenic blood product usage and can have a positive effect on patient outcomes. The flow rates are under 700 cc/minute. Our more…

Edwards Lifesciences Technology Sarl +1-(949)-250-2500

Medrad, Inc. www.medrad.com

Warrendale, Pennsylvania Medrad, Inc. deals in medical devices and services that enable & enhance imaging procedures of the human body. We are engaged in the production of vascular injection systems for diagnostic or interventional procedures. We manufacture and market a complete line of CT injection systems. We also offer more…

Boston Scientific Corporation www.bostonscientific.com

Natick, Massachusetts Boston Scientific Corporation specializes in the development, manufacturing and marketing of medical devices. We also design and produce cardiovascular medical products. Our cardiovascular division concentrates on providing medical treatment to cardiovascular, peripheral vascular & neurovascular dis more…

Venetec International, Inc. venetec.com

Biosensors Intl. Pte. Ltd. www.biosensors.com

Singapore Biosensors Intl. Pte. Ltd. serves as the manufacturing centre for critical care products such as embolectomy catheters, thermodilution catheters,and central venous catheters. more…

Senko Medical Trading Co. www.senko-trd.co.jp

Japan Senko Medical Trading Co. distributes medical products. We focus on cardiothoracic, surgical products, anesthesia, and otolaryngologic products. more…

Invatec Innovative Technologies, S.R.L. www.invatec.com

Italy Invatec Innovative Technologies, S.R.L. is a producer of catheters. Our coronary products include Falcon CTO, Piccolo, Bravo, Grande & Forte, Avion plus, Skylor and Skipper. Our peripheral products are Hippocampus, Scuba, Admiral xtreme, Maris plus & deep. Our Falcon CTO balloon catheter provides so more…

3by Ltd. www.3by.com

Israel 3by Ltd. specializes in turn-key projects of medical components, devices and systems. We provide clean room production, sophisticated plastic injection molding services, technical design assistance, assembly and product testing. Our solutions include injection, automatic assembly, product testing an more…

Pfm Produkte für die Medizin AG www.pfm-ag.de

Germany Pfm Produkte für die Medizin AG is a marketing and sales specialist for medical technology products in the fields of pathology/histology, OP/anesthesia, infusion therapy & interventional technologies. We offer various products including anterior chamber cannulas, anti roll device sets, aprons, arter more…

Intra Special Catheters GmbH www.intra-online.de

Dispomedica GmbH www.dispomedica.de

Germany Dispomedica GmbH deals with healthcare products under categories such as anesthesia, neuro surgery, cardio surgery and sterilization. The ventricular catheters are designed for temporary drainage of cerebrospinal fluid (CSF), in order to reduce and control intracranial pressure. The temporary myocar more…

Vascutech, Inc. +33-(800)-628-9470

France Vascutech, Inc. provides vascular balloon catheter and biliary catheter. more…

Occlusion catheter suppliers

Lemaitre Vascular, Inc. www.lemaitre.com

Catheter Research, Inc. (CRI) www.catheterresearch.com

Indianapolis, Indiana Catheter Research, Inc. (CRI) is a manufacturer and developer of medical devices. We specialize in catheters, tubing and OEM medical device manufacturing. We have numerous patents describing various catheters and similar medical devices with single and multiple elements of shape memory nitinol. The more…

Telemed Systems Inc. www.telemedsystems.com

Hudson, Massachusetts Telemed Systems Inc. is manufacturer of medical accessory devices which are utilized with the flexible endoscope in the field of gastroenterology. Our product line includes polypectomy snares, gastrointestinal cytology brushes, bronchial cytology brushes, balloon catheters, disposable sclerotherapy more…

Boston Scientific Corporation www.bostonscientific.com

Dispomedica GmbH www.dispomedica.de

Billary stents

Vitae Core www.vitaecore.com

Cypress, California Vitae Core is a specialized medical device company involved in the marketing and distribution of OEM/branded products. We offer urology, radiology, gastroenterology, braces/back supports, scissors and dental instruments. Our urology products include urethral balloon catheter, slings, nephrostomy bal more…

Cordis Corp. +1-(786)-313-2000

Polymerex Medical Corp. www.polymerex.com

San Diego, California Polymerex Medical Corp. specializes in providing PTCA, PTA balloon catheters, stents and accessories. We also offer variety of components including tubing, medical balloon, luer and hub. We provide plastics, lubricious & heat shrink tubing, biliary, esophageal & tracheal stent, torque device and ins more…

Flexible Stenting Solutions, Inc. www.flexiblestent.com

Eatontown, New Jersey Flexible Stenting Solutions, Inc. is engaged in the business of stents. Our stenting solutions technology is designed for the harsh loading conditions in the superficial femoral and popliteal arteries, which are in the dominant sites and peripheral vascular diseases. Our fully connected stent has co more…

Allwin Medical Devices, Inc. www.allwinmedical.com

Anaheim, California Allwin Medical Devices, Inc. manufactures urology products. Our urology products include biopsy needles, dilators, guidewires, stone buster pneumatic lithotripters, meatal dilators and urinary diversion stents. We offer needles, catheters, drainage sets, speciality stents, stent removers, stone bask more…

Cordis Corporation, A Johnson & Johnson Co. www.cordis.com

Warren, New Jersey Cordis Corporation, A Johnson & Johnson Co. is a developer and manufacturer of breakthrough stents, catheters and guidewires for interventional medicine, minimally invasive computer-based imaging, and electrophysiology. We offer products for cardiology, endovascular, and biliary. Our brands include more…

Idev Technologies, Inc. www.idevtechnologies.com

Houston, Texas Idev Technologies, Inc. supplies medical device products designed for endovascular interventional use. Our Supera® transhepatic biliary stent uses the novel wire interwoven nitinol (WIN) design which offers great conformity to the natural biliary duct and 1:1 nominal sizing. Above or below the k more…

Medi-Globe Corporation www.mediglobe.com

Tempe, Arizona Medi-Globe Corporation is a developer, manufacturer and distributor of instruments, catheters, devices, implants & equipment for flexible endoscopy, urology, cardiology and wound care. We also distribute a wide range of hospital supplies. We focus on the minimally invasive surgical market with speci more…

Hobbs Medical Inc. www.hobbsmedical.com

Stafford Springs, Connecticut Hobbs Medical Inc. specializes in the design and development of diagnostic & therapeutic accessories for the gastrointestinal & pulmonary market. Our achalasia balloon dilator is manufactured from specially treated polyurethane. It has standard luer-lock fittings for compatibility with inflation/def more…

Bard Peripheral Vascular, Inc. www.bardpv.com

Tempe, Arizona Bard Peripheral Vascular, Inc. deals with vascular products. Our product list comprises of abdominal/thoracic grafts, hemodialysis access grafts, peripheral bypass grafts, stents, stent grafts, and venacava filters. The LifeStent® vascular stent has a combination of helical structures, encompass more…

Boston Scientific Corporation www.bostonscientific.com

Abbott Laboratories www.abbott.com

Abbott Park, Illinois Abbott Laboratories is a diversified health care company which discovers, develops, manufactures and markets innovative products & services that span the continuum of care from prevention, diagnosis to treatment & cure. We focus on advancing medical science & the practice of health care with experti more…

Guidant Corporation www.guidant.com

Olympus KeyMed Ltd. www.keymed.co.uk

Essex, United Kingdom Olympus KeyMed Ltd. manufactures and supplies specialized medical & industrial equipments. We manufacture high-quality electro-optical products, such as cameras & microscopes and endoscopic instrumentation for both medical & industrial applications. Our product categories are laparo-endoscopic singl more…

ACE Medical Devices Pvt. Ltd.SEND INQUIRY

Maharashtra, India Ace Medical Devices Pvt. Ltd. manufactures and distributes medical devices. We are an ISO 9001:2001 and ISO 13485 certified company. Our products are CE-certified in accordance with MDD 93/42/EEC. We offer urology & gastro disposables, and disposable laparoscopic scissors. Our products include ureth more…

Manish Medi-Innovation saimanish.com

Karnataka, India Medi-Innovation produces super specialty surgical disposables in the field of urology, gynaecology and gastroenterology. We deal in stents, catheters, dilators, guide wire, graspers, IP needles, penile clamps, stone baskets and rigid graspers. Endoscopic biliary stents, endoscopic biliary drainage c more…

Aster Medispro Pvt Ltd www.astermedispro.net

Karnataka, India Aster Medispro produces medical devices in the specialities of urology, radiology, gastroenterology and gynaecology. Our products include PCN catheter, malecot catheter, suprapublic catheter, prostatic stent, ureteral dilator, stone basket, stone grasper, loop stent, and tieman. Our urethral indwell more…

Medi-Globe GmbH www.medi-globe.de

Germany Medi-Globe GmbH produces and distributes minimal-invasive instruments & accessories used in the fields of gastroenterology & flexible endoscopy. We also deal with wound care systems. We have DIN EN ISO 13485: 2003 certification to our credit. Some of our products are biopsy forceps, foreign body ret more…

Taewoong Medical Co., Ltd www.stent.net

Korea, Republic Of Taewoong Medical Co., Ltd develops stents. Our GI stents are used to maintain or restore the lumen of hollow organs, vessels, and ducts. Non-vascular stents are devices to create an artificial pathway, open for hollow lumen organs that are closed or obstructed due to cancerous lesions or benign dise more…

Medinol Ltd. www.medinol.com

Israel Medinol Ltd. specializes in the manufacture of cardiology products with the invention of the flexible closed cell stent design. We focus on the stent technology to combine thicker and thinner strut to optimize the balance between flexibility and scaffolding. Our product line comprises of Nirflex® more…

Carotid shunts suppliers

C. r. Bard, Inc. www.crbard.com

Murray Hill, New Jersey C. r. Bard, Inc. manufactures and markets life-enhancing medical technologies in the fields of vascular, urology, oncology & surgical specialty products. We are an ISO 9000 certified company. We offer products by business unit, disease state, process listing, idea generation process, OEM & E commerc more…

Bard Electrophysiology www.bardep.com

Lemaitre Vascular, Inc. www.lemaitre.com

Perouse Medical www.perouse.com

France Perouse Medical specializes in cardiovascular surgery, oncology and interventional imaging fields. Our products for cardiovascular surgery include knitted and woven polyester vascular prostheses, balloon catheters, carotid shunts and vein strippers. Our implantable catheter port is flexible and with more…

External and internal carotid shunts suppliers

Sophysa USA, Inc. www.sophysa.com

Crown Point, Indiana Sophysa USA, Inc. specializes in adjustable valves. Our lumbo-peritoneal catheter kit is a complete set that ensures drainage of cerebrospinal fluid (CSF) from the subarachnoid space of the spine to a sophy valve & from the valve to the peritoneal cavity. Our Pulsar® valve is endowed with a one way device & allows patency checking & CSF access & is available in 2 sizes and 3 pressure ranges. Our infusion sets to be used with Soph-A-Port implantable access port are available, simple or with l more…

Lemaitre Vascular, Inc. www.lemaitre.com

Burlington, Massachusetts LeMaitre Vascular, Inc. is a global provider of devices for the treatment of peripheral vascular disease. We develop, manufacture, and market disposable & implantable vascular devices to address the needs of vascular surgeons & interventionalists. Our product portfolio consists of brand name products used in arteries and veins outside of the heart. We offer stent grafts, biologic vascular patch, carotid shunts, covered stents, contrast injector, and implantable ports. The UniFit aorto-uni-iliac more…

Micro vascular clips suppliers

Roboz Surgical Instrument Co., Inc. www.roboz.com

Gaithersburg, Maryland Roboz Surgical Instrument Co., Inc. specializes in providing hand-crafted surgical instruments. Our surgical instruments include tweezers & forceps, bone instruments, surgical & vascular clips & clamps, scalpels, retractors, wound closure & vascular access instruments, instrument care & handling pro more…

Stoelting Co. www.stoeltingco.com

Wood Dale, Illinois Stoelting Co. produces and distributes instruments for basic biomedical research in neuroscience & physiology. Our ANY-maze™ is a flexible video tracking system designed to automate testing in behavioural experiments more…

Aesculap Inc. www.aesculapusa.com

Center Valley, Pennsylvania Aesculap Inc. manufactures surgical instrumentation. Our products include surgical instruments, laparoscopy, endoscopy, neurosurgery, sutrures, surgical quality management, and consulting services. Our cardiovascular instruments includes peripheral vascular, aorta, anastomosis clamps, vascular clips more…

Lemaitre Vascular, Inc. www.lemaitre.com

RZ-Medizintechnik Gmbh www.rz-medizintechnik.com

Germany RZ-Medizintechnik GmbH offers standard and speciality instruments & accessories for various surgical fields such as arthroscopy, ENT, urology, ophthalmology, & plastic surgery. We offer a complete set of laryngoscopes for adults and children. These laryngoscopes permit a good view of the laryngeal a more…

Stainless steel tunneler vascular graft suppliers

Teleflex Medical www.teleflexmedical.com

Research Triangle Park, North Carolina Teleflex Medical, a division of Teleflex Incorporated, is a supplier of medical devices, surgical instruments & disposable medical products. We are a global outsource provider that focuses on medical devices and orthopedic surgical instruments. Our OEM brands include Beere Medical, KMedic, Deknatel more…

Lemaitre Vascular, Inc. www.lemaitre.com

C. R. Bard, Inc., Bard Medical Div. www.bardmedical.com

Covington, Georgia C. R. Bard, Inc., Bard Medical Div. provides products and services that meet the needs of healthcare providers & patients. We specialize in disease state management offering the industry’s comprehensive product inventory for patient care. We offer a full line of Foley catheters including infection c more…

Zeppelin Medical Instruments Ltd. www.zeppelin.md

Germany Zeppelin Medical Instruments Ltd. produces and distributes medical products. Our haematoscope is designed for neuro endoscopic surgery where a large working channel and best image information is needed. Our trepanmotor is designed in particular for the cranial burr hole trepanation at low speed. Our more…

General Surgical Co., (india) Pvt. Ltd. www.gescoindia.com

Tamil Nadu, India General Surgical Co., (india) Pvt. Ltd. is a manufacturer of surgical instruments. We produce medical & surgical disposables, general, ENT, neuro & spinal, orthopedic, gynecology & obstetrics, plastic, cardio thoracic, urology, oncology, vascular, ophthalmic, dental, oral & maxillofacial surgery ins more…

Baur Und Haselbarth-Chirurg Gmbh www.bh-chirurg.de

Germany Baur Und Haselbarth-Chirurg GmbH is a manufacturer of surgical instruments. We manufacture a broad variety of surgical instruments including aspiration & suction instruments, atomizers, ear specula, gynecological instruments, retractors, trachea tubes and rectal instruments. Our aspiration & suction more…

Vascular stent suppliers

DRG International, Inc. www.drg-international.com

Mountainside, New Jersey DRG International, Inc. is a multinational specialty medical equipment and diagnostics manufacturer & distributor. We offer products for enzyme immunoassays, rapid saliva & tumor tests, radio immunoassays & lab equipments. Our enzyme immunoassays include adrenocorticotropic hormone, alpha fetoprotei more…

Atrium Medical Corporation www.atriummed.com

Cordis Corp. +1-(786)-313-2000

Vascular Architects, Inc.SEND INQUIRY

San Jose, California Vascular Architects, Inc. designs, manufactures and markets instrumentation used in the treatment of vascular stenoses, occlusions and non-vascular obstructions. A key area of emphasis is the treatment of peripheral vascular disease, which manifests itself as a reduction or loss of blood flow due to more…

Lemaitre Vascular, Inc. www.lemaitre.com

Fort Wayne Metals www.fwmetals.com

Fort Wayne, Indiana Fort Wayne Metals specializes in the research, development and production of fine grade medical wire. We work with stainless steel, titanium and titanium alloys and specialty alloys such as nitinol. Our products include flat and shaped wires, center less and precision ground bar, drawn filled tubing more…

Bard Peripheral Vascular, Inc. www.bardpv.com

Micro-tech (Nanjing) Co., Ltd. www.micro-tech.cn/indexen.htm

Jiangsu, China Micro-tech (Nanjing) Co., Ltd develops, manufactures & distributes stents series products, biopsy forceps and other medical devices for minimal invasive operation. We perform sterilization inspection for our single use medical devices. Our product line includes biliary duct, colonic, duodenal, esoph more…

Tayside Flow Technologies Limited www.tayflow.com

United Kingdom Tayside Flow Technologies Limited focuses on the development of vascular devices. We offer vascular devices that are based on blood flow dynamics spiral laminar flow technology. Our SLF™ spiral grafts are monitored by conventional techniques to determine the effects on the pressure and flow ch more…

Cardio-Nef, S.A. De C.V. www.cardionef.com

N.L., Mexico Cardio-Nef, S.A. De C.V. provides coronary stent, guide wire catheter and catheter introducer. more…

Taewoong Medical Co., Ltd www.stent.net

Contech Medical International, Ltd. www.contechireland.com

Ireland Contech Medical International, Ltd. is an OEM sub-contract manufacturer servicing the medical device industry. We offer OEM medical device assembly & packaging, winged infusion and straight needle sets, both uncoated & coated balloon, stent protectors, catheter & guide wire dispensers. Our technical more…

Micro-Tech (Nan Jing) Co., Ltd. www.stent.cc

China Micro-Tech (Nan Jing) Co., Ltd. manufactures & distributes stent series products, biopsy forceps and medical devices for minimally invasive operations. We perform sterilization inspection for single use medical devices. Our product line comprises of biliary duct, colonic, duodenal, esophageal, prost more…

Cardiopulmonary bypass vascular catheter suppliers

Autosuture www.autosuture.com

Norwalk, Connecticut Autosuture offers a complete line of surgical products and instrumentation that surgeons utilize for laparoscopic, endoscopic & traditional open surgical procedures & lymphatic mapping. We are an ISO 9001, ISO 9002, CE MARK certified company. We offer products like endo catch™ 10mm specimen bag, end more…

Chase Medical www.chasemedical.com

Richardson, Texas Chase Medical designs & manufactures products for the comprehensive surgical treatment of congestive heart failure, including products for surgical ventricular restoration procedures and for both beating heart & traditional CABG procedures. We offer products such as catalyst, Marisa™, Mannequin & PT more…

Abiomed, Inc. www.abiomed.com

Danvers, Massachusetts Abiomed, Inc. develops & distributes heart assist and replacement systems. We offer healthcare professionals an array of choices across a broad clinical spectrum from the catheterization lab to the surgical suite, together with interventional cardiologists and surgeons. Our AbioCor is a completely s more…

Cook Group Incorporated www.cookgroup.com

Viasys Healthcare Inc www.viasyshealthcare.com

San Diego, California Viasys Healthcare Inc. develops & distributes technology medical devices that are used in respiratory care, neurology, vascular medicine and critical care. Our Infant Flow® SiPAP™ renders bi-level nasal CPAP for the spontaneously breathing neonate through delivery of sighs above a baseline more…

Edwards Lifesciences Corporation www.edwards.com

Medtronic Xomed Surgical Products, Inc www.xomed.com

Integra LifeSciences Corporation www.integra-ls.com

Plainsboro, New Jersey Integra LifeSciences Corporation develops & markets surgical instruments, as well as devices and products for use in neurosurgery, reconstructive surgery, general surgery and soft tissue repair. Our Samy™ vascular retractors enable the neurosurgeon to elevate, retract and depress the vessel, t more…

Luxtec www.luxtec.com

West Boylston, Maryland Luxtec produces medical illumination systems. We develop lighting and visualization systems for the operating room. Our products include headlights, ultralite, halogen, camera, surgical loupes, monitors, printers, and light sources. Our ultralite consists of ergonomic designs that use the head’s nat more…

Medtronic, Inc. www.medtronic.com

Vortex Medical Inc www.angiovac.com

Norwell, Massachusetts Vortex Medical Inc specializes in novel endomechanical devices for the endovascular market. We provide AngioVac® cannula and circuit. It is a novel catheter-based device that facilitates the suction, filtering, and simultaneous reinfusion of blood. The AngioVac® cannula, a unique balloon-act more…

Endoscopic Technologies, Inc. www.estech.com

San Ramon, California Endoscopic Technologies, Inc. develops medical devices and disposables that enable cardiac surgeons to perform a variety of traditional and minimally invasive surgical procedures. Our Cobra Adhere XL™ surgical system is a minimally invasive epicardial probe that utilizes ten electrodes to crea more…

Global Blood Resources, Llc +1-(800)-9429243

Windsor, Connecticut Global Blood Resources, Llc offers cardiopulmonary bypass blood reservoir and cardiopulmonary bypass vascular catheters. more…

Pemco, Inc. www.pemcomed.com

Cleveland, Ohio Pemco, Inc. is a manufacturer of precision surgical instruments that include custom perfusion systems. Our products include anesthesia shield, suction handles, suction sets, suction tips, cannula connectors, heart pumps and retractors. Our anesthesia shield provides a protective area around the pati more…

Cardeon Corp. +1-(408)-253-3319

Cupertino, California Cardeon Corp. specializes in providing various catheters, cannula & tubing, vascular and cardiopulmonary bypass products. more…

Cardiac Assist, Inc. www.cardiacassist.com

Pittsburgh, Pennsylvania CardiacAssist, Inc. develops, manufactures and markets medical device products to provide cardiologists and cardiac surgeons. Our product range includes tandemheart cannula set, tandemheart controller and tandemheart system pump. Our tandemheart transseptal cannula set-enhanced flow 72 provides exte more…

Circulatory Technology, Inc. www.cirtec.com

Oyster Bay, New York Circulatory Technology, Inc. develops medical devices to improve the safety and efficacy of cardiopulmonary bypass. Our products include The Better-Bladder™ (BB), The V-Bag™, The Better-Header™ and The Better-Venter™. The Better-Bladder™ (BB) is an inline reservoir that more…

Lemaitre Vascular, Inc. www.lemaitre.com

Cascade Life Solutions, LLC +1-(616)-977-2505

Grand Rapids, Michigan Cascade Life Solutions, LLC are providers of tourniquet kit with snares, cardioplegia cannulae, sucker and cardiovascular accessories. more…

Avalon Laboratories, Inc. www.avalonlabs.com

Rancho Dominguez, California Avalon Laboratories, Inc. is a supplier of wire-reinforced catheters and cannulae. Our products include vascular access kits, bi-caval dual lumen and multi-port venous femoral catheters. The bi-caval dual lumen catheter is a single site, kink resistant, veno-venous device designed to enable optimal more…

Voss Medical Products vossmedicalproducts.com

San Antonio, Texas Voss Medical Products is a medical device developer/specifier specializing in surgical products. Our product categories are positioning, cardiovascular and specialty. We offer positioning devices, and graft markers, cannulas, and clamps used in coronary bypass procedures. Our single use disposable P more…

Alliant Healthcare Products www.allianthealthcare.com

Richland, Michigan Alliant Healthcare Products designs, develops, manufactures and markets products for the healthcare market. We also provide custom assembly, packaging and manufacturing for acute care hospitals, government & original equipment (OEM) for private label customers. We focus on cardiovascular, general su more…

Vitalcor, Inc. www.vitalcor.com

Westmont, Illinois Vitalcor, Inc. manufactures and distributes medical devices used primarily in cardio-thoracic surgery. We specialize in coronary artery perfusion cannulae with balloon. The balloon is made of self-inflating PVC with no latex. more…

Atek Medical www.atekmedical.com

Grand Rapids, Michigan Atek Medical is a producer of medical products. We manufacture class II and III disposable, implantable and electro-mechanical devices. We have extensive assembly capabilities that include UV bonding, ultrasonic welding, pad printing, laser marking, FFS packaging, tray sealing, bar sealing, catheter more…

Shelhigh, Inc. www.shelhigh.com

Union, New Jersey Shelhigh, Inc. offers SemiStented™ aortic tricuspid valves, stentless aortic valves, stentless valve conduit, and tricuspid valves. The NR2000 stentless aortic valves offers supravalvular implantation using single layer continuous suture line. It requires no rinsing and is available in a wide more…

California Medical Laboratories www.calmedlab.com

Costa Mesa, California California Medical Laboratories develops, distributes and manufactures cardiovascular cannulation products. Our product line includes cardiovascular cannulation products, cardioplegia products, vent catheters, suction wands, beating heart products, custom cannulation kits & accessories. Our custom c more…

Surge Medical Solutions, LLC. www.surgemedical.com

Grand Rapids, Michigan Surge Medical Solutions, LLC. provides solution for cardiovascular surgery, emergency services and emergency preparedness as well as a variety of other healthcare markets. Our retrograde provides the means for delivering cardioplegia solution to the patient’s heart. The cannulae permit delivery of c more…

Bard Shannon Limited +1-(908)-277-8000

Humacao Bard Shannon Limited supplies medical devices and diagnostic equipments. Our product line includes biopsy systems, mesh bags and precision pass. more…

Churchill Medical Systems, Inc. www.churchillmedicalsystems.com

Montgomeryville, Pennsylvania Churchill Medical Systems, Inc. is a manufacturer of procedure kits, IV sets and accessories, TPN bags & pharmacy admixture products. We offer a complete custom product program. Our extension sets include standard bore extension sets, micro bore extension sets, minibore & ultra-microbore extension s more…

C. R. Bard, Inc., Bard Medical Div. www.bardmedical.com

Jostra Bentley, Inc. +1-(302)-454-9959

Anasco Jostra Bentley, Inc. offers various surgical and disposable medical products. We provide arterial filters, blood infusion line, cardioplegia cooling/administration set, cardiotomy venous reservoirs, custom cardiovascular perfusion kits, disposable sucker, oxygen saturation meter, pleural drainage/au more…

Vygon Corp. www.vygonusa.com

Norristown, Pennsylvania Vygon Corp. deals with single-use medical and surgical products. Our neonatal & pediatric special care products are categorized as vascular access, digestive tract and respiratory tract. The PremiCath is a 27G (1.1 Fr) Flexane® catheter for mid-long term I.V.therapy. Its 24G splitting introducer more…

Clinical Instruments Intl., Inc. +1-(508)-764-2200

Southbridge, Massachusetts Clinical Instruments Intl., Inc. provides carotid bypass shunt, introducers and detergent reagent. more…

Terumo Medical Corporation +1-(410)-392-7243, 800-283-7866

Elkton, Maryland Terumo Medical Corporation deals with blood specimen collection devices, coaxial introducers, entry needles, guide wires, phlebotomy needle cap holders, and piston syringes. more…

Sorin Group USA, Inc. www.soringroup-usa.com

Terumo Cardiovascular Systems www.terumo-cvs.com

Ann Arbor, Massachusetts Terumo Cardiovascular Systems (TCVS) develops, manufactures and distributes medical devices for cardiac & vascular surgery with an emphasis on cardiopulmonary bypass, intra–operative monitoring & vascular grafting. The Fresenius continuous autotransfusion system (C.A.T.S) salvages red blood cells fo more…

Atrion Medical Products, Inc. www.atrionmedical.com

Arab, Alabama Atrion Medical Products, Inc., a division of Atrion Corporation specializes in medical devices. Our product lines provide solutions for a variety of medical markets such as cardiovascular, orthopedic, ophthalmic, urological and anesthesia. Our QL® inflation device is perfect for a wide array of more…

Smiths Medical ASD, IncSEND INQUIRY

Smiths Medical Deutschland GmbH www.smiths-medical.com/de

Germany Smiths Medical Deutschland GmbH provides medical devices for the hospital, emergency, home and specialist environments. Our Point-Lok® device is a needle safety solution for needles found in epidural, spinal and other procedural trays. Our BCI® 3301 pulse oximeter and Digit™ finger pul more…

Erika De Reynosa, S.A. De C.V. +52-(899)-921-3500

Mexico Erika De Reynosa, S.A. De C.V. specializes in offering orthopedic, prosthetic and surgical appliances & supplies. Our products include tubing clamps, catheter connectors, I.V. administration sets, single needle blood sets & accessories, and various types of blood tubing sets, transducer protectors f more…

Kelsar, S.A. +52-(0)-89-41-86

Mexico Kelsar, S.A. specializes in offering catheter bags, intraventricular probes and oxygen & bag feeder. Our Argyle DeLee suction catheter with mucous trap is intended to aspirate liquids or semisolids from a patient’s upper airway. more…

Terumo Corporation www.terumo.co.jp

Tokyo, Japan Terumo Corporation manufactures & distributes medical products & equipment that include pharmaceuticals, nutritional food supplement, blood bags, disposable medical devices, cardiovascular systems, peritoneal dialysis, blood glucose monitoring system, medical electronic and digital thermometers. Our more…

Dideco S.P.A. www.sorin-cp.com

MO, Italy Dideco S.P.A. focuses on perfusion and blood management systems. Our products include endoscopic vessel harvesting, cardiopulmonary equipment, oxygenators, optimized bypass systems, venous and cardiotomy reservoirs, arterial filters, cardioplegia, hemoconcentration, monitoring, centrifugal blood pum more…

Sorin S.p.A.SEND INQUIRY

Italy Sorin S.p.A. focuses on the development of products used to treat cardiovascular and renal diseases. Our product categories are endoscopic vessel harvesting, cardiopulmonary equipments, oxygenators, arterial filters and cannulae & suckers. Our ClearGlide® ERA for endoscopic radial harvesting ena more…

DMC Medical Ltd. www.dmcmedical.net

Ireland DMC Medical Ltd. offers manufacturing, consultancy and distribution service to the medical device sector. Our product list comprises of saphenous vein distention systems, cardiac insulation pads, vein irrigation cannulas, and polycarbonate connectors. The saphenous vein distention system (SVDS) prev more…

Admedes Schuessler Gmbh www.admedes.com

Germany Admedes Schuessler Gmbh provides nitinol self expandable components to medical industries. Our product line comprises of nitinol stents, percutaneous heart valve frames, filters, occlusion devices and distal protection devices. We also specialize in laser cuttings, shape settings, surface finishes, more…

Maquet Cardiopulmonary Ag www.maquet-cp.com

Germany Maquet Cardiopulmonary Ag is a provider of medical technology for emergency rooms, operating rooms and intensive care units. We offer complete solutions for operating theatres and intensive care units. We supply OR tables, lights and complete OR solutions. Endoscopic vessel harvesting or EVH is a pr more…

Bionic Medizintechnik GmbH www.bionic-jms.com

Taunus, Germany Bionic Medizintechnik GmbH specializes in the distribution of dialysis and transfusion products. We also manufacture catheters and therapy chairs & beds. We offer a wide range of medical single-use products. We supply blood bags and equipments needed for blood transfusion. Demers-Katheter® is a more…

Vygon S A www.vygon.com

France Vygon S A offers single use medical and surgical products. We focus on urinary tract surgery, wound drainage, digestive tract, respiratory tract, neonatology, and operation theater products. Our urinary tract products include pediatric vesical catheters, rectal catheters, hourly diuresis and urine d more…

Allegiance Healthcare Corp. 847-473-1500

Dominican Republic Allegiance Healthcare Corp are providers of introducer needle reusables, disposable bome marrow biopsy needles and trays. more…

Davis And Geck Caribe, Ltd. 203-845-1000

Dominican Republic Davis And Geck Caribe, Ltd. specializes in the production of polytetrafluorethylene pledget, disposable endoscopic specimen pouch, steel sutures and umbilical tape-sterile round cotton tape. more…

Cardiomed Supplies Inc. www.cardiomed.com

Ontario, Canada Cardiomed Supplies Inc. is a manufacturer and distributor of disposable surgical products. We supply disposable products for open heart surgery, critical care, dialysis, and oncology. Our comprehensive product line includes renal and peritoneal dialysis catheters, catheters for intensive and critica more…

Coronary stent graft system suppliers

TriReme Medical, Inc. www.trirememedical.com

Pleasanton, California TriReme Medical, Inc. specializes in providing products for physicians to use in the treatment of coronary artery disease. We offer Antares™ coronary stent system and Glider™ PTCA balloon catheter. Our Glider™ PTCA balloon catheter can be used to dilate highly-stenosed lesions. more…

Elixir Medical Corporation www.elixirmedical.com

Sunnyvale, California Elixir Medical Corporation develops products that combine medical devices with pharmaceuticals to provide treatment solutions. Drug-eluting stent systems are designed to optimize localized drug delivery to provide a safe treatment for cardiovascular patients. Our coronary stent is manufactured from more…

Lemaitre Vascular, Inc. www.lemaitre.com

Abbott Hematology www.abbott.us

Santa Clara, California Abbott Hematology offers pharmaceutical, medical, and nutritional products. Our product range comprises of medicines, medical diagnostic instruments & tests, minimally invasive surgical devices, and a spectrum of nutritional supplements for infants, children & adults. Our perclose A-T suture medicat more…

Medtronic Neurosurgery +1-(901)-344-0645 , 800-468-9710

Goleta, California Medtronic Neurosurgery deals with cranial neurosurgery market. Our products include a wide variety of PS Medical® silicone elastomer valves, catheters, & shunts for hydrocephalus management, neuroendoscopes for improved surgical access and cranial closure products for quick & secure reattachment more…

Catheter tip occluder suppliers

Teleflex Medical www.teleflexmedical.com

Cook Group Incorporated www.cookgroup.com

Medtronic Xomed Surgical Products, Inc www.xomed.com

Lemaitre Vascular, Inc. www.lemaitre.com

Clinical Instruments Intl., Inc. +1-(508)-764-2200

Southbridge, Massachusetts Clinical Instruments Intl., Inc. provides carotid bypass shunt, introducers and detergent reagent. more…

Applied Medical www.appliedmedical.com

Codan Medical Aps www.codan.de

Denmark Codan Medical Aps is a manufacturer of disposable medical transfer systems. Our products include infusion sets, transfusion sets, I.V. accessories, pediatric products, syringes, I.V. pumps and continence care products. more…

Synthetic/biological composite vascular graft suppliers

Datascope Corp. www.datascope.com

Fairfield, New Jersey Datascope Corp. offers intervascular and cardiac assist products. We offer balloon pumps, balloon catheters, sutureless securement devices, vascular grafts and peripheral stents. Our CS300 balloon pump with IntelliSense™ combines fiber-optic speed with automatic in vivo calibration. The result more…

Atrium Medical Corporation www.atriummed.com

Lemaitre Vascular, Inc. www.lemaitre.com

Maquet Inc. www.maquet.com

Wayne, New Jersey Maquet Inc. designs equipment and disposables for cardiac surgery. We provide products for ventilation, perfusion systems, cardiac surgery and cardiopulmonary products. We also produce different types of operating tables and lights. more…

Boston Scientific Corporation www.bostonscientific.com

Terumo Corporation www.terumo.co.jp

Perouse Medical www.perouse.com

Bionova International Pty. Ltd. www.bionova.com.au

VIC, Australia Bionova International Pty. Ltd. manufactures vascular prostheses. Our Omniflow II is a biosynthetic vascular prosthesis fpr peripheral revascularization and arteriovenous access. Our research and testing laboratories are equipped to conduct many specialized evaluations on the physico-chemical charac more…

Valvulotome suppliers

Koven Technology, Inc. www.koven.com

St. Louis, Missouri Koven Technology, Inc offers healthcare products. We are an ISO certified company. Our HD-307 is a versatile bi-directional surgical doppler & has a special single frequency unit created for optimal sound quality in low flow states. Our echosounder ES-102EX is a heavy-duty desktop fetal doppler that more…

Edwards Lifesciences Corporation www.edwards.com

Scanlan International www.scanlaninternational.com

St. Paul, Minnesota Scanlan International designs and manufactures surgical instrumentation. Our product categories are cardiac/vascular, neurosurgical, single-use products, instrument care and custom design. Our Scanlan® single-use aorta/vein punches have large finger rings for greater control & accuracy and taper more…

Instrumed International, Inc. www.instrumedinc.biz

Schaumburg, Illinois Instrumed International, Inc. specializes in providing reusable surgical instruments. We offer surgical products for bipolar, CV/thoracic, ENT, general, hand & micro surgery, laparoscopic, laryngeal, maxillo-facial, neuro/spine, OB/GYN, ophthalmic, orthopedic, plastics and urology. We also carry a b more…

Lemaitre Vascular, Inc. www.lemaitre.com

Uresil, LLC www.uresil.com

Skokie, Illinois Uresil, LLC is a medical device development, manufacturing and distribution company that serves the needs of physicians who perform minimally invasive procedures. Our products are categorized into interventional radiology and surgical products. Some of our products are catheter with locking pigtail, more…

Geister Medizintechnik GmbH www.geister.com

Olympus Imaging Corporation www.olympus.co.jp

Japan Olympus Imaging Corporation specializes in medical endoscopes and surgical products,artificial bone replacement material and dental products. We also deal with microscopes and the medical information systems program. The Evis Lucera upper alimentary canal general-purpose video scope corresponds to n more…

Dimeda Instrumente Gmbh www.dimeda.de

Germany Dimeda Instrumente Gmbh specializes in surgical instruments. We offer products for endoscopy, neurosurgery, cardiovascular surgery, gynecology, orthopedics and plastic surgery. Our product list comprises of laryngoscopes, aneurysm vessel clips, saw & power tools, and nasopharyngolaryngoscopes. Our e more…

Guided wires

http://www.neometricsinc.com/technologies.html

Medical Guidewire Expertise from Design Through ManufacturingNeoMetrics Minneapolis, MNare the experts in manufacturing OEM mandrel guide wires and wire-based OEM medical devices. NeoMetrics offers medical guide wires for OEM medical procedures. We specialize in FDA cleared steerable guide wires and nitinol guide wires for OEM medical devices.

Guided Wires MA based

Techdevice Corporation www.techdevice.com

Watertown, Massachusetts Techdevice Corporation manufactures balloons, catheters, coils, ground cores and finished guidewires. We specialize in the development of custom medical balloons. Our balloons are ideal for PTCA and PTA catheters, stent delivery systems, esophageal & endotrachial applications and spine therapies. We more…

Biosphere Medical, Inc. www.biospheremed.com

Rockland, Massachusetts Biosphere Medical, Inc. focuses on applying proprietary microsphere technology to medical applications using embolotherapy techniques. Our core technologies, consisting of patented bio-engineered polymers and manufacturing methods, are used to produce miniature spherical beads with beneficial proper more…

Navilyst Medical, Inc. www.navilystmedical.com

Marlborough, Massachusetts Navilyst Medical, Inc. offers medical devices for vascular access, and for the diagnosis & treatment of vascular disease. Our products are used by various healthcare providers including interventional radiologists, interventional cardiologists, oncologists, surgeons, IV nurses & oncology nurses. We more…

Guidewire Technologies, Inc. guidewiretech.com

Salem, New Hampshire Guidewire Technologies, Inc. offers medical guidewires. Our guidewires come in standard, fixed core, and custom designs. Our capabilities include spring winding, grinding, welding, marking, j-tip forming, and PTFE coating. more…

Angiotech Pharmaceuticals, Inc. www.angiotech.com

Vancouver Angiotech Pharmaceuticals, Inc. is a global specialty pharmaceutical and medical device company that discovers, develops, & markets innovative technologies & medical products primarily for local diseases or for complications associated with medical device implants, surgical interventions & acute inj more…

Pace Medical, Inc. www.pacemedicalinc.com

Waltham, Massachusetts Pace Medical, Inc. is involved in designing and marketing a complete line of high-quality temporary cardiac pacing products. Our products include both single and dual-chamber temporary cardiac pacemakers, a dual-chamber pacing analyzer, autoclavable temporary pacemaker extension and surgical cables, more…

Concert Medical www.concertmedical.com

Norwell, Massachusetts Concert Medical provides interventional cardiology products. We offer conductor guidewire family and regional anesthesia products. We provide BSmart™, injection monitor for use in regional anesthesia. It has been designed to provide significant clinical information at a fantastic value. more…

Advanced Biomedical Devices, Inc. (ABD, Inc.) www.abd-inc.com

Andover, Massachusetts Advanced Biomedical Devices, Inc. (ABD, Inc.) provides contract engineering and design. We offer medical grade gas dispenser for balloon inflation with CO2 and CO2 powered injector for thermal dilution. This is useful for filling balloons especially for pediatric and adult procedures, whenever there more…

Radius Medical Technologies, Inc. www.radiusmed.com

Acton, Massachusetts Radius Medical Technologies, Inc. specializes in design, development and marketing of minimally invasive medical devices for treating cardiovascular diseases. Our Expro™ elite snare has a 0.035″ profile that permits delivery through conventional diagnostic or therapeutic catheters elimina more…

Rocket Medical www.rocketmedical.com

Hingham, Massachusetts Rocket Medical deals with products for cardiac and thoracic drainage, ascites drainage, infertility, labor ward, colposcopy, and sterile supplies. Our Rocket® Genesis™ embryo transfer catheter set has a new inner catheter design combined with an ultra smooth tip profile that reduces the ri more…

Boston Scientific Corporation www.bostonscientific.com

Ovalum Ltd. www.ovalum.net

Israel Ovalum Ltd. develops and implements effective and safe solutions for chronic and acute total occlusions in the coronary and peripheral arteries. Based on proprietary shape memory alloy techniques and laser processes we offer systems for minimally-invasive cardiology and interventional radiology fiel more… Ovalum Ltd. develops and implements effective and safe solutions for chronic and acute total occlusions in the coronary and peripheral arteries. Based on proprietary shape memory alloy techniques and laser processes we offer systems for minimally-invasive cardiology and interventional radiology fields. The minimally-invasive solution, the citop™ guidewire system, was created for the treatment of arterial conditions that today require bypass surgery or amputation of the lower limb. Our products citop™ 10 CTO Crossing System is a complete platform for CTO cross-over, traverse™ micro-catheter is a 1.9F (0.025”) micro-catheter for easy penetration & octobooster™ is an extension wire.

Aortic Valve

Cryolife Inc. www.cryolife.com

Kennesaw, Georgia CryoLife® Inc. is a biomedical company that produces low temperature preservation of human tissues for implant. Our CryoLife-O’Brien® stentless aortic porcine valve is made of three non-coronary leaflets & is implanted with a single suture line technique. Our BioGlue® surgical adhesive i more…

Carbomedics Inc. www.carbomedics.com

Austin, Texas Carbomedics Inc. specializes in the development of products for treatment of valvular heart disease. We focus on products used to treat cardiovascular & renal diseases. Our OrbisTM universal aortic and mitral valve have a multipurpose cuff design, which allows for a variety of implantation technique more…

St. Jude Medical, Inc. www.sjm.com

St. Paul, Minnesota St.Jude Medical, Inc. delivers implantable bradycardia, cardiac surgical, electrophysiology, implant cardiac monitors, repair, tachycardia, tissue valves, spinal cord stimulation, patient care network, mechanical valves, cardioverter defibrillators, pacemakers, electrophysiology catheters, vascular more…

Edwards Lifesciences Corporation www.edwards.com

Nucleus Medical Art Inc. www.nucleusinc.com

Kennesaw, Georgia Nucleus Medical Art Inc. creates and/or licenses medical illustrations, medical animations, medical images, anatomical charts, anatomical models and interactive multimedia for educational and commercial use. We maintain a proprietary database of more than 15,000 highly detailed, expert reviewed medi more…

Direct Flow Medical, Inc. www.directflowmedical.com

Santa Rosa, California Direct Flow Medical, Inc. deals with aortic tissue valve prosthesis. Our aortic tissue valve prosthesis provides treatment for cardiac valve insufficiency with a safe and effective percutaneous option. more…

On-X Life Technologies, Inc www.onxlti.com

Austin, Texas On-X Life Technologies, Inc manufactures the On-X® Prosthetic Heart Valve. Our heart valve is a pure carbon bileaflet heart valve prosthesis. The smooth surfaces of pure carbon, a transitional flare at the inlet and sleek interior contours of the valve diminish the principal causes of turbulence more…

ATS Medical, Inc. www.atsmedical.com

Minneapolis, Minnesota ATS Medical, Inc. caters to the requirements of the cardiovascular surgery market, providing life-sustaining solutions for cardiac surgeons and their patients. Our products include ATS Open Pivot® heart valves, ATS 3f® aortic bioprosthesis, ATS simulus® annuloplasty valve repair rings/bands and ATS more…

Shelhigh, Inc. www.shelhigh.com

Sorin Biomedica Cardio S.p.A. www.sorin-cid.com

Via Crescentino, Italy Sorin Biomedica Cardio S.p.A. specializes in the field of high-technology bioengineering. We manufacture heart valves. Our bicarbon slimline valve is designed for supra-annular placement of the whole sewing cuff. Our soprano aortic bioprosthesis is created for a totally supra-annular seating, which more…

Minogue Medical, Inc. www.minogue-med.com

Quebec, Canada Minogue Medical, Inc. is engaged in the production of surgical robot. We offer da Vinci ® surgical robot that enables surgeons to control every aspect of surgery. Our da Vinci ® prostatectomy offers robotic surgery for prostate cancer or robotic prostatectomy. It is a minimally invasive surg more…

Mitral Valve

Carbomedics Inc. www.carbomedics.com

St. Jude Medical, Inc. www.sjm.com

Edwards Lifesciences Corporation www.edwards.com

Nucleus Medical Art Inc. www.nucleusinc.com

On-X Life Technologies, Inc www.onxlti.com

Shelhigh, Inc. www.shelhigh.com

Thomas Medical Products, Inc. www.thomas-medical.com

Malvern, Pennsylvania Thomas Medical Products, Inc. is a medical device manufacturer. We design and develop Class II and Class III single-use devices for OEM customers. We focus on catheter based vascular access and vascular device delivery medical devices for diagnostic and therapeutic procedures in the cardiology, elec more…

Landmark Surgical Ltd www.landmark-surgical.co.uk

Merseyside, United Kingdom Landmark Surgical Ltd supplies a wide range of surgical instruments. We offer a wide range of quality instruments for minimally invasive surgery. Our cardio thoracic instruments include forceps, artery forceps, coronary artery bypass retractors, hand held retractors, bulldog clamps, dilators, corona more…

Sorin Biomedica Cardio S.p.A. www.sorin-cid.com

Kaisers Surgical Instruments Pty Ltd www.kaisers.com.au

Minogue Medical, Inc. www.minogue-med.com

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Archive for the ‘CABG’ Category

Assessing Cardiovascular Disease with Biomarker

A Changing expectation from cardiac biomarkers.

Historical perspective

References

A Metabolic Functional Meaning of Existence of Isoenzymes

References

Fundamental Transformative Concepts Carried Over from Physics to Biomolecular Processes.

References

A New Imperative

Cardiovascular Biomarkers

I. BNP:

[A] Aids in the Prevention of Cardiac Events by Detecting Silent Ischemic Lesions and Selecting Patients for Imaging

[B] Evaluating CHF patients in the emergency department

Open Journal of Clinical Diagnostics scirp.org

ABSTRACT

We observe the following changes with respect to NT-proBNP and age:

Adjustment of the NT-proBNP for eGFR and for age over 50 difference

Renal Effect on NT-proBNP

[E] Mid-region proANP in Emergency Room

II. CRP

[A] Predictor of benefit of lowering CRP with statin

[B] Predictor of cardiovascular disease

__________________________________________________________________________________________________________________________

III. Troponin(s) and hs-TnI/cTnT

________________________________________________________________________________________________________________________________________________________________________

IV. Predicting cardiovascular mortality in NSTEMI patients

______________________________________________________________________________________________________________________________________________________

V. Assessing Cardiovascular Risk

Related articles

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CABG or PCI: Patients with Diabetes – CABG Rein Supreme

Compelling Evidence for Coronary-Bypass Surgery in Patients with Diabetes

SOURCE INFORMATION

REFERENCES

Related Research on this Open SOurce On-Line Scientific Journal include the following:

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To Stent or Not? A Critical Decision

Fractional Flow Reserve–Guided PCI versus Medical Therapy in Stable Coronary Disease

BACKGROUND

METHODS

RESULTS

CONCLUSIONS

SOURCE INFORMATION

Conclusions

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Prematurely halted ALTITUDE trial showed When added to monotherapy with either an ACE inhibitor or an angiotensin receptor blocker (ARB), aliskiren (Tekturna) did not improve outcomes in patients with type 2 diabetes who had high cardiovascular and renal risk

ESC: Aliskiren Onboard No Help in T2D

Aliskiren

Adverse effects

Contraindications

Drug interactions

References

External links

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ESC: New Definition of MI Unveiled

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Competition in the Ecosystem of Medical Devices in Cardiac and Vascular Repair: Heart Valves, Stents, Catheterization Tools and Kits for Open Heart and Minimally Invasive Surgery (MIS)

This report covers the following product categories

Heart Valve Frames:

Stents:

Surgical tools:

The ecosystem of Cardiac and Vascular Surgery for Repair or Replacement by Implantation of a new blood vessel or medical device covers the following procedure-related devices and tools now in use:

Product Category Total US and Total Global Suppliers, Suppliers in MA by Product, Segment Industry Concentration in the US and in MA

Industry Segment Concentration Ratio: Impact on Market Penetration Cost and Potential Revenue and Market Share per Product Line

Penetration Strategy for a Global Supplier Targeting the US Market and the Massachusetts Market

Customized predictions of penetration cost and estimation of potential revenues based on the industry segment concentration ratios in the Table above are part of an Actionable Strategic Market Entry Plan into the US market.

Contact Us

National Medical Device Suppliers within the Cardiac and Vascular Repair Market by Product Category

Cardiology vascular surgery – The OR equipment

Arterial catheterization kit suppliers

Embolectomy catheters suppliers

Arrow Internacional De Mexico, S.A. De C.V. +52-(610)-378-0131