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阿司匹林摄入对健康受试者血小板衍生微囊泡的影响。

Effect of acetylsalicylic acid intake on platelet derived microvesicles in healthy subjects.

机构信息

Department of Neurology, Poznan University of Medical Sciences, Poznan, Poland.

Laboratory of Flow Cytometry and Vascular Biology, Department of Neurology, Poznan University of Medical Sciences, Poznan, Poland.

出版信息

Platelets. 2020;31(2):206-214. doi: 10.1080/09537104.2019.1588242. Epub 2019 Mar 21.

Abstract

Platelet-derived microvesicles (pMVs) are released from platelets in physiological and pathological conditions and exhibit a wide range of prothrombotic, antithrombotic, proatherogenic, and pro-inflammatory properties. Antiplatelet agents, such as acetylsalicylic acid (ASA), are widely used for the prevention and treatment of vascular diseases, but their impact on pMV release remains poorly understood and contradictory mainly because of discrepancies in the methodology and lack of well-standardized MV assessment protocols. The present study investigated the effects of ASA not only on total pMV release but also on their phenotypes defined using the surface expression of pro-inflammatory (CD40L, CD62P, CD31) and procoagulant (PS, PAC-1) markers in healthy subjects. Fifty healthy volunteers were enrolled in the study and received a daily dose of 150 mg ASA for 3 consecutive days. Circulating pMVs were characterized and quantified before and after the intervention period using flow cytometry. Serum levels of thromboxane B2 (TXB2) and whole blood impedance platelet aggregation under arachidonic acid (AA) stimulation were also investigated to assess ASA compliance. In general, ASA did not effect pMV numbers in healthy subjects despite its effective inhibition of platelet aggregation Moreover, in premenopausal women, we noticed an increase in the number of pMVs. Further studies are needed to assess whether dose modification of ASA or combinations or changes in antiplatelet therapy would reduce pMV formation, especially in patients with cardiovascular risk factors.

摘要

血小板衍生的微泡 (pMVs) 在生理和病理条件下从血小板中释放出来,并表现出广泛的促血栓形成、抗血栓形成、促动脉粥样硬化和促炎特性。抗血小板药物,如乙酰水杨酸 (ASA),被广泛用于预防和治疗血管疾病,但它们对 pMV 释放的影响仍知之甚少且存在矛盾,主要是由于方法学上的差异以及缺乏标准化的 MV 评估方案。本研究不仅研究了 ASA 对总 pMV 释放的影响,还研究了其对健康受试者中炎症(CD40L、CD62P、CD31)和促凝(PS、PAC-1)标志物表面表达定义的表型的影响。50 名健康志愿者入组本研究,并连续 3 天每天服用 150mg ASA。在干预前后使用流式细胞术对循环 pMVs 进行特征和定量分析。还研究了血清血栓素 B2 (TXB2) 水平和全血在花生四烯酸 (AA) 刺激下的阻抗血小板聚集,以评估 ASA 依从性。总的来说,尽管 ASA 有效抑制了血小板聚集,但它并没有影响健康受试者的 pMV 数量。此外,在绝经前妇女中,我们注意到 pMV 数量增加。需要进一步研究评估 ASA 剂量调整或联合或改变抗血小板治疗是否会减少 pMV 形成,特别是在心血管危险因素患者中。

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