Residual platelet thromboxane A2 and prothrombotic effects of erythrocytes are important determinants of aspirin resistance in patients with vascular disease

Background: Permanent inactivation of cyclooxygenase‐1 and inhibition of platelet thromboxane A₂ (TxA₂) constitute the main mechanisms underlying the prevention of vascular disease by aspirin. Methods and Results: We studied platelet TxA₂ synthesis and its impact on platelet reactivity and platelet–erythrocyte platelet‐rich plasma (PRP)–RBC] interactions in 533 aspirin‐treated patients with vascular disease. Seventy aspirin‐free and 16 aspirin‐treated normal subjects were evaluated as controls. Collagen (1 μg mL^?1)‐induced platelet activation (¹⁴C‐5HT release) and recruitment (proaggregatory activity of cell‐free releasates from activated platelets) were assessed in PRP, PRP + RBC, and whole blood (WB). TxA₂ was quantified in releasates from WB. Aspirin inhibited TxA₂ synthesis and platelet function in all patients, but to different degrees. Forty‐two patients (8%) displayed partial (<95%) inhibition of TxA₂ relative to that of aspirin‐free controls. They produced >3.5 ng mL^?1 TxA₂ and had higher platelet reactivity than 491 patients who had undetectable TxA₂ or produced residual TxA₂ (R‐TxA₂; ≤3.5 ng mL^?1). Patients with R‐TxA₂ were distributed into TxA₂ quartiles. Patients in the third and fourth quartiles had significantly elevated ¹⁴C‐5HT release in PRP, which was markedly amplified in PRP + RBC and WB. TxA₂ in the fourth quartile translated into increased platelet aggregation and recruitment. Significant correlations were found between R‐TxA₂ and platelet hyperfunction. Conclusion: Biochemical markers (TxA₂ synthesis, ¹⁴C‐5HT release) and biological assays (platelet aggregation and recruitment) used to monitor the aspirin effect in a large population of patients presenting with vascular disease have evidenced the importance of R‐TxA₂ and the prothrombotic effects of RBC in aspirin resistance.