Article date: April 2008
By: Anneke Bierend, Thomas Rau, Renke Maas, Edzard Schwedhelm, Rainer H. Böger, in Volume 65, Issue 4, pages 540-547
What is already known about this subject
Aims
Recently, two genetic polymorphisms of the platelet ADP receptor P2Y12 (haplotypes H2 and 34T) have been implicated in increased platelet aggregation and atherothrombotic risk. It was suggested that these polymorphisms contribute to a diminished response to antiplatelet drugs. Therefore, we investigated the effects of these polymorphisms on platelet aggregation in aspirin‐treated patients with coronary artery disease (CAD).
Methods
Platelet aggregation was studied in platelet‐rich plasma from 124 patients with CAD treated with 100 mg aspirin day−1. P2Y12 ADP receptor polymorphisms were determined by PCR‐RFLP. The 52G > T polymorphism was used as tag‐SNP for the H2 haplotype. Aggregation was induced by 1 mg l−1 collagen. In a subgroup (n = 72), a concentration‐response curve to collagen (0.5–10 mg l−1), aggregation at 2 μmol l−1 ADP and 1 mmol l−1 arachidonic acid were determined.
Results
Whereas arachidonic acid‐induced aggregation was inhibited in all patients, collagen and ADP‐induced aggregation were highly variable. However, aggregation did not differ significantly between carriers and noncarriers of the 52T‐allele (1 mg l−1 collagen: 32.7% (21.9–38.6%) vs. 32.5% (21.2–41.6%); P = 0.77; ADP: 33.1% (29.9–40.9%) vs. 39.1% (31.5–49.7%); P = 0.34), respectively. EC50 values were 1.26 mg l−1 (0.79–2.02) and 1.54 mg l−1 (0.98–2.4) collagen in noncarriers and carriers of the H2 haplotype, respectively (P = 0.56). Moreover, the 34°C > T polymorphism did not significantly affect any of the aggregatory responses.
Conclusions
Low‐dose aspirin inhibits platelet aggregation to the same extent in patients carrying or not carrying the P2Y12 H2 haplotype and/or the 34T allele. Our data do not support the hypothesis that these polymorphisms contribute to an attenuated antiplatelet effect of aspirin.
DOI: 10.1111/j.1365-2125.2007.03044.x
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