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首页> 外文期刊>Thrombosis Research: An International Journal on Vascular Obstruction, Hemorrhage and Hemostasis >Enhanced platelet sensitivity to prostacyclin in patients in an active stage of Takayasu arteritis.
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Enhanced platelet sensitivity to prostacyclin in patients in an active stage of Takayasu arteritis.

机译:高发性动脉炎活跃期患者对前列环素的血小板敏感性增强。

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Patients in an active stage of Takayasu arteritis are often complicated with thrombosis in the affected vessels. We investigated whether alteration of platelet sensitivity to prostacyclin is involved in platelet function in these patients. Twelve female patients in an active stage (48.3+/-11.8 years, mean+/-S.D.), diagnosed clinically by a persistently elevated erythrocyte sedimentation rate (>40 mm/h) with typical symptoms, along with 10 gender- and age-matched patients in an inactive stage and 12 control subjects were enrolled. Half-maximal concentration (EC(50)) for platelet aggregation to collagen was determined in the presence and absence of 1 nM iloprost, a stable prostacyclin analog. Sensitivity of platelets to prostacyclin was quantified by the ratio of EC(50) (R) in the presence of iloprost to that in its absence. Patients in an active stage exhibited enhanced platelet aggregation, as demonstrated by significantly lower EC(50) to collagen and increased plasma thromboxane B(2) concentration. However, R values in these patients were significantly higher (4.00+/-1.05; P<.001) than those in the inactive patients or controls (2.58+/-0.62 and 2.43+/-0.68, respectively), suggesting enhanced sensitivity to prostacyclin in patients with active disease. Plasma 6-keto-PGF1 alpha levels were lower in the active patients than those in other groups of subjects. We conclude that platelets in an active stage of TA may be sensitive not only to collagen but also to prostacyclin. The increase in sensitivity of the platelets to prostacyclin could be a compensatory mechanism against a decrease in the prostanoid production, presumably associated with endothelial dysfunction.
机译:高隆动脉炎活跃期的患者通常会在受影响的血管中并发血栓形成。我们调查了这些患者中血小板对前列环素敏感性的改变是否与血小板功能有关。十二个处于活动阶段的女性患者(48.3 +/- 11.8岁,平均+/- SD),通过典型症状的持续性红细胞沉降率(> 40 mm / h)以及10个性别和年龄相匹配的临床诊断为临床处于不活动状态的患者和12名对照受试者入组。在存在和不存在1 nM iloprost(一种稳定的前列环素类似物)的情况下,确定血小板聚集至胶原蛋白的半数最大浓度(EC(50))。血小板对前列环素的敏感性通过存在伊洛前列素与不存在伊洛前列素时的EC(50)(R)之比来定量。处于活动期的患者表现出增强的血小板凝集,这表现为胶原蛋白的EC(50)明显降低,血浆血栓素B(2)浓度升高。然而,这些患者的R值显着高于非活动患者或对照组的R值(4.00 +/- 1.05; P <.001)(分别为2.58 +/- 0.62和2.43 +/- 0.68),表明对活动性疾病患者的前列环素。活动患者的血浆6-酮-PGF1α水平低于其他受试者组。我们得出结论,处于TA活动期的血小板可能不仅对胶原蛋白敏感,而且对前列环素敏感。血小板对前列环素敏感性的增加可能是针对前列腺素生成减少(可能与内皮功能障碍有关)的一种补偿机制。

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