Kinetics and prognostic value of soluble VCAM‐1 in ST‐segment elevation myocardial infarction patients

Ahmad Hayek; Alexandre Paccalet; Laura Mechtouff; Claire C. Da Silva; Fabrice Ivanes; Hadrien Falque; Simon Leboube; Yvonne Varillon; Camille Amaz; Charles deBourguignon; Cyril Prieur; Danka Tomasevic; Nathalie Genot; François Derimay; Eric Bonnefoy‐Cudraz; Gabriel Bidaux; Nathan Mewton; Michel Ovize; Thomas Bochaton

doi:10.1002/iid3.409

Immunity, Inflammation and Disease (Jun 2021)

Kinetics and prognostic value of soluble VCAM‐1 in ST‐segment elevation myocardial infarction patients

Ahmad Hayek,
Alexandre Paccalet,
Laura Mechtouff,
Claire C. Da Silva,
Fabrice Ivanes,
Hadrien Falque,
Simon Leboube,
Yvonne Varillon,
Camille Amaz,
Charles deBourguignon,
Cyril Prieur,
Danka Tomasevic,
Nathalie Genot,
François Derimay,
Eric Bonnefoy‐Cudraz,
Gabriel Bidaux,
Nathan Mewton,
Michel Ovize,
Thomas Bochaton

Affiliations

Ahmad Hayek: Intensive Cardiological Care Division, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Alexandre Paccalet: INSERM U1060, CarMeN Laboratory University of Lyon, Groupement Hospitalier Est Bron France
Laura Mechtouff: Department of Neurology and Stroke Center, Hospices Civils de Lyon Lyon University Lyon France
Claire C. Da Silva: Intensive Cardiological Care Division, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Fabrice Ivanes: Faculty of Medicine, Loire Valley Cardiovascular Collaboration University of Tours Tours France
Hadrien Falque: Department of Cardiology, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Simon Leboube: Intensive Cardiological Care Division, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Yvonne Varillon: Clinical Investigation Center and Heart Failure Department, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Camille Amaz: Clinical Investigation Center and Heart Failure Department, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Charles deBourguignon: Clinical Investigation Center and Heart Failure Department, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Cyril Prieur: Intensive Cardiological Care Division, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Danka Tomasevic: Intensive Cardiological Care Division, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Nathalie Genot: Intensive Cardiological Care Division, Louis Pradel Hospital Hospices Civils de Lyon Bron France
François Derimay: Department of Cardiology, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Eric Bonnefoy‐Cudraz: Intensive Cardiological Care Division, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Gabriel Bidaux: INSERM U1060, CarMeN Laboratory University of Lyon, Groupement Hospitalier Est Bron France
Nathan Mewton: Clinical Investigation Center and Heart Failure Department, Louis Pradel Hospital Hospices Civils de Lyon Bron France
Michel Ovize: INSERM U1060, CarMeN Laboratory University of Lyon, Groupement Hospitalier Est Bron France
Thomas Bochaton: Intensive Cardiological Care Division, Louis Pradel Hospital Hospices Civils de Lyon Bron France

DOI: https://doi.org/10.1002/iid3.409
Journal volume & issue: Vol. 9, no. 2
pp. 493 – 501

Abstract

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Abstract Background Soluble vascular cell adhesion molecule‐1 (sVCAM‐1) is a biomarker of endothelial activation and inflammation. There is still controversy as to whether it can predict clinical outcome after ST‐elevation myocardial infarction (STEMI). Our aim was to assess the sVCAM‐1 kinetics and to evaluate its prognostic predictive value. Method We prospectively enrolled 251 consecutive STEMI patients who underwent coronary revascularization in our university hospital. Blood samples were collected at admission, 4, 24, 48 h and 1 month after admission. sVCAM‐1 serum level was assessed using ELISA assay. All patients had cardiac magnetic resonance imaging at 1‐month for infarct size (IS) and left ventricular ejection fraction (LVEF) assessment. Clinical outcomes were recorded over 12 months after STEMI. Results sVCAM‐1 levels significantly increased from admission up to 1 month and were significantly correlated with IS, LVEF, and LV end‐systolic and diastolic volume. (H48 area under curve (AUC) ≥ H48 median) were associated with an increased risk of adverse clinical events during the 12‐month follow‐up period with a hazard ratio (HR) = 2.6 (95% confidence interval [CI] of ratio = 1.2–5.6, p = .02). The ability of H48 AUC for sVCAM‐1 to discriminate between patients with or without the composite endpoint was evaluated using receiver operating characteristics with an AUC at 0.67 (0.57–0.78, p = .004). This ability was significantly superior to H48 AUC creatine kinase (p = .03). Conclusions In STEMI patients, high sVCAM‐1 levels are associated with a poor clinical outcome. sVCAM‐1 is an early postmyocardial infarction biomarker and might be an interesting target for the development of future therapeutic strategies.

Published in Immunity, Inflammation and Disease

ISSN: 2050-4527 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: https://onlinelibrary.wiley.com/journal/20504527

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