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Consistent platelet inhibition during long-term maintenance-dose clopidogrel therapy among 359 compliant outpatients with documented vascular disease - 09/08/11

Doi : 10.1016/j.ahj.2006.12.006 
Victor L. Serebruany, MD, PhD a, , Alex I. Malinin, MD a, Dan Atar, MD b, Dan F. Hanley, MD a
a HeartDrug Research Laboratories, Johns Hopkins University, Towson, MD 
b Division of Cardiology, Aker University Hospital, University of Oslo, Oslo, Norway 

Reprint requests: Victor L. Serebruany, MD, PhD, HeartDrug Research Laboratories, Osler Medical Bldg, 7600 Osler Drive, Suite 307, Towson, MD 21204.

Riassunto

Background

Numerous reports have dichotomized responses after clopidogrel therapy using varying definitions and platelet tests in patients immediately after acute vascular events; however, no large study has assessed platelet characteristics in outpatients receiving long-term treatment for more than 30 days with the maintenance dose (75 mg/d) of clopidogrel. The aim of this study was to describe the responses of ex vivo measures of platelet aggregation and activation to long-term clopidogrel therapy in a large population of outpatients after coronary stenting or ischemic stroke.

Methods

We conducted a secondary post hoc analysis of a data set represented by presumably compliant patients after coronary stenting (n = 237) or a documented ischemic stroke (n = 122) treated with clopidogrel-and-aspirin combination antiplatelet therapy.

Results

The mean duration of treatment was 5.8 months (range 1-21 months). Every patient exhibited a significant inhibition of adenosine diphosphate–induced platelet aggregation (mean 52.9%, range 36%-70%) as compared with the preclopidogrel measures. Inhibition of aggregation strongly correlated with a diminished expression of PECAM-1 (platelet/endothelial cell adhesion molecule 1, r = 0.75), glycoprotein IIb/IIIa (r = 0.62), and PAR-1 (protease-activated receptor 1, r = 0.71). None of the patients developed hyporesponsiveness (reduction from the baseline <15%) or profound inhibition (residual platelet activity <10%).

Conclusions

In contrast to the wide variability of responses that exists in the acute setting, long-term therapy with clopidogrel leads to consistent and much less variable platelet inhibition. Lack of nonresponse and profound inhibition with clopidogrel allow for the maintenance of a delicate balance between proven efficacy and acceptable bleeding risks for long-term secondary prevention in outpatients after acute vascular events.

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 The present analysis was not supported by external funding. The primary studies in the coronary stenting and poststroke cohorts were supported by the Sanofi-BMS Partnership (New York, NY), Pfizer (New York, NY), Boehringer-Ingelheim (Ingelheim, Germany), Novartis (Basel, Switzerland), and Eli Lilly (Indianapolis, IN). DA was supported by a grant from the National Association of Norway for Public Health–the Norwegian Council for Heart and Vessels, the Eastern Regional Health Authority of Norway, and the Aker University Hospital Research Foundation.


© 2007  Mosby, Inc. Tutti i diritti riservati.
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Vol 153 - N° 3

P. 371-377 - marzo 2007 Ritorno al numero
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