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每日阿司匹林治疗与非 COX-1 依赖性血小板功能的时间依赖性变化。

Time-dependent changes in non-COX-1-dependent platelet function with daily aspirin therapy.

机构信息

Institute for Genome Sciences and Policy, Duke University, 905 S. Lasalle Dr., DUMC Box 3445, Durham, NC 27710, USA.

出版信息

J Thromb Thrombolysis. 2012 Apr;33(3):246-57. doi: 10.1007/s11239-012-0683-0.

Abstract

To develop an integrated metric of non-COX-1-dependent platelet function (NCDPF) to measure the temporal response to aspirin in healthy volunteers and diabetics. NCDPF on aspirin demonstrates wide variability, despite suppression of COX-1. Although a variety of NCDPF assays are available, no standard exists and their reproducibility is not established. We administered 325 mg/day aspirin to two cohorts of volunteers (HV1, n = 52, and HV2, n = 96) and diabetics (DM, n = 74) and measured NCDPF using epinephrine, collagen, and ADP aggregometry and PFA100 (collagen/epi) before (Pre), after one dose (Post), and after several weeks (Final). COX-1 activity was assessed with arachidonic acid aggregometry (AAA). The primary outcome of the study, the platelet function score (PFS), was derived from a principal components analysis of NCDPF measures. The PFS strongly correlated with each measure of NCDPF in each cohort. After 2 or 4 weeks of daily aspirin the Final PFS strongly correlated (r > 0.7, P < 0.0001) and was higher (P < 0.01) than the Post PFS. The magnitude and direction of the change in PFS (Final–Post) in an individual subject was moderately inversely proportional to the Post PFS in HV1 (r = -0.45), HV2 (r = -0.54), DM (r = -0.68), P < 0.0001 for all. AAA remained suppressed during aspirin therapy. The PFS summarizes multiple measures of NCDPF. Despite suppression of COX-1 activity, NCDPF during aspirin therapy is predictably dynamic: those with heightened NCDPF continue to decline whereas those with low/normal NCDPF return to pre-aspirin levels over time.

摘要

开发一种综合的非 COX-1 依赖的血小板功能(NCDPF)指标,以测量健康志愿者和糖尿病患者中阿司匹林的时间反应。尽管 COX-1 受到抑制,但阿司匹林的 NCDPF 显示出广泛的可变性。尽管有多种 NCDPF 检测方法,但尚无标准,其重复性也未得到证实。我们给两组志愿者(HV1,n = 52;HV2,n = 96)和糖尿病患者(DM,n = 74)服用 325 mg/天的阿司匹林,并用肾上腺素、胶原和 ADP 聚集度和 PFA100(胶原/肾上腺素)在(Pre)、一剂后(Post)和数周后(Final)测量 NCDPF。用花生四烯酸聚集度(AAA)评估 COX-1 活性。研究的主要结果是血小板功能评分(PFS),它来自 NCDPF 测量的主成分分析。在每个队列中,PFS 与 NCDPF 的每个测量值都有很强的相关性。在每天服用阿司匹林 2 或 4 周后,Final PFS 与每个队列中的每个 NCDPF 测量值都有很强的相关性(r > 0.7,P < 0.0001),且高于 Post PFS(P < 0.01)。个体受试者中 PFS 的变化幅度和方向(Final-Post)与 HV1 中的 Post PFS 呈中度负相关(r = -0.45),HV2(r = -0.54),DM(r = -0.68),P < 0.0001。在阿司匹林治疗期间,AAA 仍受到抑制。PFS 概括了多种 NCDPF 测量值。尽管 COX-1 活性受到抑制,但阿司匹林治疗期间的 NCDPF 是可预测的动态变化:那些 NCDPF 升高的人继续下降,而那些 NCDPF 低/正常的人随着时间的推移恢复到阿司匹林前的水平。

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