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基础血小板活性增加、血浆脂联素水平升高以及糖尿病与血小板对阿司匹林体外效应的反应性差有关。

Increased basal platelet activity, plasma adiponectin levels, and diabetes mellitus are associated with poor platelet responsiveness to in vitro effect of aspirin.

作者信息

Takahashi Shinichi, Ushida Miho, Komine Risa, Shimizu Aya, Uchida Toshihiro, Ishihara Hiroaki, Shibano Toshiro, Watanabe Gentaro, Ikeda Yasuo, Murata Mitsuru

机构信息

The Keio Daiichi Project on Genetics of Thrombosis, Keio University, Tokyo, Japan.

出版信息

Thromb Res. 2007;119(4):517-24. doi: 10.1016/j.thromres.2006.04.004. Epub 2006 Jun 21.

Abstract

INTRODUCTION

Aspirin is one of the most effective antiplatelet agents and is now commonly used to prevent vascular events. In some patients, however, recurrent vascular events have been demonstrated despite aspirin therapy. Our objective was to characterize individuals showing poor response to in vitro effect of aspirin, using PFA-100.

METHODS

One hundred sixty-eight healthy male subjects were analyzed. We assessed platelet function tests, including PFA-100, whole blood aggregation, and optical platelet aggregation. Also measured were hemostatic and other parameters including von Willebrand factor (VWF:Ag), VWF ristocetin cofactor activity (VWF:RCo), soluble vascular adhesion molecule-1 (sVCAM-1), high sensitive C-reactive protein (hs-CRP), and adiponectin. Poor responders were defined as having a collagen/epinephrine-induced closure time (CEPI-CT) under 250 s with PFA-100 when incubated with 10 microM aspirin, whereas good responders were defined as having a CEPI-CT of more than 250 s.

RESULTS AND CONCLUSIONS

PFA-100 tests revealed that 40 subjects (24%) were poor responders (PR) and 128 (76%) were good responders (GR). Poor responsiveness was significantly associated with (1) higher basal platelet activities in PFA-100, as well as in whole blood aggregation and aggregometer;(2) increased level of adiponectin (8.8+/-4.1 micro g/mL [PR] vs 7.3+/-2.9 micro g/mL [GR], p=0.010);and (3) the presence of diabetes mellitus (17.5% [PR] vs 4.7% [GR], p=0.009). Importantly, whereas 24% of the subjects showed insufficient inhibition in PFA-100 when incubated with 10 microM aspirin, almost all subjects showed maximum inhibition with 30 microM aspirin. These observations suggest that higher doses of aspirin might overcome aspirin resistance.

摘要

引言

阿司匹林是最有效的抗血小板药物之一,目前常用于预防血管事件。然而,在一些患者中,尽管使用了阿司匹林治疗,仍有血管事件复发。我们的目标是使用PFA-100来表征对阿司匹林体外作用反应不佳的个体。

方法

对168名健康男性受试者进行分析。我们评估了血小板功能测试,包括PFA-100、全血凝集和光学血小板凝集。还测量了止血和其他参数,包括血管性血友病因子(VWF:Ag)、VWF瑞斯托霉素辅因子活性(VWF:RCo)、可溶性血管细胞粘附分子-1(sVCAM-1)、高敏C反应蛋白(hs-CRP)和脂联素。反应不佳者定义为在与10微摩尔阿司匹林孵育时,使用PFA-100检测胶原/肾上腺素诱导的封闭时间(CEPI-CT)低于250秒,而反应良好者定义为CEPI-CT超过250秒。

结果与结论

PFA-100测试显示,40名受试者(24%)为反应不佳者(PR),128名(76%)为反应良好者(GR)。反应不佳与以下因素显著相关:(1)PFA-100以及全血凝集和凝集仪中较高的基础血小板活性;(2)脂联素水平升高(8.8±4.1微克/毫升[PR]对7.3±2.9微克/毫升[GR],p=0.010);(3)糖尿病的存在(17.5%[PR]对4.7%[GR],p=0.009)。重要的是,虽然24%的受试者在与10微摩尔阿司匹林孵育时在PFA-100中显示抑制不足,但几乎所有受试者在30微摩尔阿司匹林时都显示出最大抑制。这些观察结果表明,更高剂量的阿司匹林可能克服阿司匹林抵抗。

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