Interindividual variability in platelet reactivity among individuals with or without antiplatelet therapy: results from a large tertiary care hospital.

IF 2.3 3区 医学 Q2 CARDIAC & CARDIOVASCULAR SYSTEMS
Journal of Thrombosis and Thrombolysis Pub Date : 2025-01-01 Epub Date: 2024-09-06 DOI:10.1007/s11239-024-03022-w
Mattia Galli, Sergio Terracina, Eleonora Schiera, Massimo Mancone, Luigi Frati, Dominick J Angiolillo, Fabio M Pulcinelli
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引用次数: 0

Abstract

Antiplatelet therapy is crucial for reducing thrombotic events in patients with atherosclerotic disease, but the response vary widely among individuals. The identification of patients at high (HPR), optimal (OPR) or low platelet reactivity (LPR) is dependent on high interlaboratory variability. We report results of a large dataset of patients to assess the gold standard light transmission aggregometry (LTA). A total of 11,913 patients who sequentially underwent LTA assessment using several stimuli (ADP-2µM, collagen-2 µg/ml, arachidonic acid 0.5 mM, epinephrine 10µM) with a standardized methodology between 2004 and 2022 were screened. After application of inclusion-exclusion criteria, 5,901 patients were included and divided into five groups: healthy-volunteers (HV; N = 534); controls (CTR; N = 1073); aspirin-treated patients (ASA; 75-150 mg/die; N = 3280); clopidogrel-treated patients (CLOP; 75 mg/die; N = 495) and patients treated with dual antiplatelet therapy, ASA plus CLOP (DAPT; N = 519). The mean PA% in response to ADP 2 μm was 72.4 ± 33.3 in the CTR population, 40.6 ± 29.9 in the ASA group, 25.1 ± 35.1 in the CLOP group and 10.2 ± 18.5 in the DAPT group. The mean PA% in response to collagen 2 ug/ml was 90.7 ± 10.5 in the CTR population, 40.8 ± 26.3 in the ASA group, 79.4 ± 21.8 in the CLOP group and 17.9 ± 19.9 in the DAPT group. The percentage of patients at OPR following ADP stimuli was 66%, 25%, and 26%, in the ASA, CLOP, and DAPT group, respectively. The percentage of patients at OPR following collagen stimuli was 56%, 22%, and 41%, in the ASA, CLOP, and DAPT group, respectively. LTA was significantly increased in response to ADP (72.4 ± 33.3vs62.7 ± 37.1; p < 0.001) and AA (90.7 ± 15.6vs87.6 ± 20.5; p < 0.001) in CTR compared to HV. Our findings support the concept that a significant proportion of individuals present a hyper- or hypo-reactive platelet phenotype potentially affecting the safety and efficacy of antiplatelet therapy. The variability in response to antiplatelet therapy was particularly evident in patients undergoing single as opposed to dual antiplatelet therapy regimens. These data support ongoing strategies of guided selection of antiplatelet therapy in patients with cardiovascular disease.

Abstract Image

接受或未接受抗血小板治疗者的血小板反应性个体间差异:一家大型三级医院的研究结果。
抗血小板治疗对减少动脉粥样硬化患者的血栓事件至关重要,但不同个体的反应差异很大。对高血小板反应性(HPR)、最佳血小板反应性(OPR)或低血小板反应性(LPR)患者的识别取决于实验室间的高变异性。我们报告了一个大型患者数据集的结果,以评估黄金标准透光聚集测定法(LTA)。2004年至2022年期间,共有11913名患者采用标准化方法(ADP-2µM、胶原蛋白-2 µg/ml、花生四烯酸0.5 mM、肾上腺素10µM)依次接受了LTA评估。在应用纳入-排除标准后,5901 名患者被纳入并分为五组:健康志愿者(HV;N = 534);对照组(CTR;N = 1073);阿司匹林治疗患者(ASA;75-150 mg/die;N = 3280);氯吡格雷治疗患者(CLOP;75 mg/die;N = 495)和接受双重抗血小板疗法(ASA 加 CLOP;DAPT;N = 519)的患者。CTR 患者对 ADP 2 μm 反应的平均 PA% 为 72.4 ± 33.3,ASA 组为 40.6 ± 29.9,CLOP 组为 25.1 ± 35.1,DAPT 组为 10.2 ± 18.5。CTR人群对胶原蛋白2微克/毫升反应的平均PA%为(90.7 ± 10.5),ASA组为(40.8 ± 26.3),CLOP组为(79.4 ± 21.8),DAPT组为(17.9 ± 19.9)。ASA 组、CLOP 组和 DAPT 组患者在受到 ADP 刺激后出现 OPR 的比例分别为 66%、25% 和 26%。ASA 组、CLOP 组和 DAPT 组患者在受到胶原刺激后出现 OPR 的比例分别为 56%、22% 和 41%。LTA对ADP的反应明显增加(72.4 ± 33.3vs62.7 ± 37.1; p
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来源期刊
CiteScore
9.20
自引率
0.00%
发文量
112
审稿时长
4-8 weeks
期刊介绍: The Journal of Thrombosis and Thrombolysis is a long-awaited resource for contemporary cardiologists, hematologists, vascular medicine specialists and clinician-scientists actively involved in treatment decisions and clinical investigation of thrombotic disorders involving the cardiovascular and cerebrovascular systems. The principal focus of the Journal centers on the pathobiology of thrombosis and vascular disorders and the use of anticoagulants, platelet antagonists, cell-based therapies and interventions in scientific investigation, clinical-translational research and patient care. The Journal will publish original work which emphasizes the interface between fundamental scientific principles and clinical investigation, stimulating an interdisciplinary and scholarly dialogue in thrombosis and vascular science. Published works will also define platforms for translational research, drug development, clinical trials and patient-directed applications. The Journal of Thrombosis and Thrombolysis'' integrated format will expand the reader''s knowledge base and provide important insights for both the investigation and direct clinical application of the most rapidly growing fields in medicine-thrombosis and vascular science.
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