Selective serotonin reuptake inhibitors yield additional antiplatelet protection in patients with congestive heart failure treated with antecedent aspirin

doi:10.1016/S1388-9842(03)00005-9

European Journal of Heart Failure 2003 5(4):517-521; doi:10.1016/S1388-9842(03)00005-9

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Selective serotonin reuptake inhibitors yield additional antiplatelet protection in patients with congestive heart failure treated with antecedent aspirin

V.L. Serebruany^a, A.H. Glassman^b, A.I. Malinin^a, D. Atar^c, D.C. Sane^d, B.R. Oshrine^a, J.J. Ferguson^e and C.M. O'Connor^f

^a Sinai Center for Thrombosis Research, Johns Hopkins University 2401 West Belvedere Avenue, Schapiro Research Building-R 202 Baltimore, MD 21215, USA
^b Columbia University New York, NY, USA
^c Frederiksberg Hospital Copenhagen, Denmark
^d Wake Forest University School of Medicine Winston-Salem, NC, USA
^e Texas Heart Institute Houston, TX, USA
^f Duke Clinical Research Institute Durham, NC, USA

^* Corresponding author. Tel.: +1-410-601-5266; fax: +1-410-601-9061 E-mail address: heartdrug{at}aol.com

Abstract

Clinical depression has been identified as an independent riskfactor for increased mortality in patients with coronary arterydisease. Enhanced platelet activity has been suggested as themechanism responsible for this adverse association. Selectiveserotonin reuptake inhibitors (SSRIs) are known to inhibit plateletsin patients undergoing coronary stenting. We sought to determinewhether concomitant therapy with SSRIs would yield additionalanti-platelet benefit in patients with congestive heart failure(CHF) already treated with antecedent aspirin. A total of 88patients with left ventricular ejection fraction (LVEF) <40%or CHF symptoms in the setting of preserved systolic functionand NYHA Class II–IV were analyzed. Of these, 23 patients(26%) were chronic SSRI users (SSRI+), and 65 patients werefree from SSRI therapy (SSRI–). All patients receivedaspirin (325 mg) for at least 1 month prior to platelet studies.Platelets were assessed by aggregometry, flow cytometry anda rapid analyzer. The SSRI+ group exhibited a substantial decreasein platelet activity when compared with SSRI– patients,as manifested by a significant reduction in ADP- (P=0.001),and collagen-induced (P=0.02) aggregation, and the expressionof PECAM-1 (P=0.03), GPIb (P=0.03), GP IIb/IIIa antigen (P=0.02)and GP IIb/IIIa activity with PAC-1 antibody (P=0.04) and P-selectin(P=0.02). Therapy with SSRIs also resulted in the reduced formationof platelet–leukocyte microparticles (P=0.01). Epinephrine-inducedaggregation in plasma, collagen-induced whole blood aggregation,closure time and expression of vitronectin receptor, CD63, CD107a,CD107b and CD151 did not differ between groups. In patientswith CHF already on aspirin, SSRI therapy was associated withfurther inhibition of platelet function. This observation mayhelp to explain some of the clinical benefits associated withSSRI therapy. Further clinical trials may help to elucidatethe potential outcome benefits of SSRIs in other potential thromboticcircumstances.

Key Words: Congestive heart failure • Platelets • Selective serotonin reuptake inhibitors (SSRIs)

Received June 11, 2002; Revised October 24, 2002; Accepted December 17, 2002

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