Aspirin nonsensitivity in patients with vascular disease: Assessment by light transmission aggregometry (aspirin nonsensitivity in vascular patients)

Hamzah Khan; Abdelrahman Zamzam; Reid C Gallant; Muzammil H Syed; Margaret L Rand; Heyu Ni; Thomas L Forbes; Mohammed Al-Omran; Mohammad Qadura

doi:10.1002/rth2.12618

Aspirin nonsensitivity in patients with vascular disease: Assessment by light transmission aggregometry (aspirin nonsensitivity in vascular patients)

Res Pract Thromb Haemost. 2021 Nov 16;5(8):e12618. doi: 10.1002/rth2.12618. eCollection 2021 Dec.

Authors

Hamzah Khan¹, Abdelrahman Zamzam¹, Reid C Gallant², Muzammil H Syed¹, Margaret L Rand³, Heyu Ni³, Thomas L Forbes⁴, Mohammed Al-Omran¹, Mohammad Qadura¹

Affiliations

¹ Division of Vascular Surgery St. Michael's Hospital Toronto ON Canada.
² Keenan Research Centre for Biomedical Science Li Ka Shing Knowledge Institute of St. Michael's Hospital Toronto ON Canada.
³ Department of Laboratory Medicine & Pathobiology University of Toronto Toronto ON Canada.
⁴ Division of Vascular Surgery Toronto General Hospital (UHN) Toronto ON Canada.

Abstract

Background: Aspirin is a key antiplatelet therapy for the prevention of thrombotic events in patients with cardiovascular disease. Studies suggest that ≈20% of patients with cardiac disease suffer from aspirin nonsensitivity, a phenomenon characterized by the inability of 81 mg aspirin to inhibit platelet aggregation and/or prevent adverse cardiovascular events.

Objectives: To investigate aspirin nonsensitivity in patients with vascular disease and assess the consequences of aspirin nonsensitivity.

Methods: One hundred fifty patients presenting to St. Michael's Hospital's outpatient clinics with evidence of vascular disease (peripheral arterial disease or carotid artery stenosis) and a previous prescription of 81 mg of aspirin were recruited in this study. Light transmission aggregometry with arachidonic acid induction was used to determine sensitivity to aspirin. Patients with a maximum aggregation ≥20% in response to arachidonic acid were considered aspirin nonsensitive, as per previous studies.

Results: Of the 150 patients recruited, 36 patients (24%) were nonsensitive to 81 mg of aspirin. Of these 36 nonsensitive patients, 30 patients provided a urine sample for urine salicyluric acid analysis (a major metabolite of aspirin). Urine analysis demonstrated that 14 patients were compliant and 16 were noncompliant with their aspirin therapy. Major adverse cardiovascular events and major adverse limb events were significantly higher in the nonsensitive patients compared to sensitive patients (hazard ratio, 3.68; P < 0.001).

Conclusion: These data highlight the high prevalence of aspirin nonsensitivity and noncompliance in patients with vascular disease and emphasizes the urgent need for improved medical management options for this patient population.

Keywords: antiplatelet; aspirin; blood platelets; platelet aggregation; thrombosis; vascular diseases.