Hematology-Oncology Section, Medical Service, Veterans Affairs Health Care System, Minneapolis, MN 55417, USA.
Clin Appl Thromb Hemost. 2012 Mar-Apr;18(2):140-9. doi: 10.1177/1076029611423387. Epub 2011 Oct 17.
We studied the ability of a new instrument, the PlaCor PRT that measures shear-induced platelet aggregation in fingerstick, non-anticoagulated blood without added agonists, to detect platelet dysfunction ex vivo. Platelet reactivity time (PRT) and whole blood aggregation (WBA) were measured in 160 healthy volunteers, before and after aspirin and in 170 participants with established vascular disease or risk factors thereof treated with aspirin ± clopidogrel. Pretreatment PRT and WBA were significantly correlated (collagen r = -.63; arachidonate r = -.65; P < .0001). Following aspirin, the mean PRT increased from 82 to 142 seconds (P < .0001), and in participants treated with clopidogrel-aspirin, the mean PRT (286 seconds, n = 65) was significantly longer than with aspirin alone (166 seconds, n = 105; P < .001). Only 13% of PRTs of participants treated with clopidogrel and aspirin were within the normal range. We conclude that the PlaCor PRT is a simple, rapid, point-of-care instrument that compares favorably with published descriptions of other platelet function instruments.
我们研究了一种新仪器,即 PlaCor PRT,它可以在非抗凝、未添加激动剂的指尖血中测量剪切诱导的血小板聚集,从而体外检测血小板功能障碍。在 160 名健康志愿者、170 名已确诊血管疾病或存在血管疾病风险因素并接受阿司匹林和/或氯吡格雷治疗的参与者中,测量了血小板反应时间 (PRT) 和全血聚集 (WBA)。预处理的 PRT 和 WBA 显著相关(胶原 r = -.63;花生四烯酸 r = -.65;P <.0001)。服用阿司匹林后,PRT 平均从 82 秒增加到 142 秒(P <.0001),在接受氯吡格雷-阿司匹林治疗的参与者中,PRT 平均(286 秒,n = 65)显著长于单独使用阿司匹林(166 秒,n = 105;P <.001)。仅 13%接受氯吡格雷和阿司匹林治疗的参与者的 PRT 值在正常范围内。我们得出结论,PlaCor PRT 是一种简单、快速、即时的仪器,与其他血小板功能仪器的已发表描述相比具有优势。
