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前列环素和伊洛前列素在周围动脉疾病患者中的纤溶活性。

Fibrinolytic activity of prostacyclin and iloprost in patients with peripheral arterial disease.

作者信息

Musiał J, Wilczyńska M, Sładek K, Cierniewski C S, Nizankowski R, Szczeklik A

出版信息

Prostaglandins. 1986 Jan;31(1):61-70. doi: 10.1016/0090-6980(86)90225-x.

Abstract

We studied the effects of prostacyclin (PGI2) and its stable analog, iloprost, on blood fibrinolytic activity in 33 patients with peripheral arterial disease. Ten subjects (group A) received three 5-hour infusions of iloprost on three consecutive days. The remaining 23 patients received three different 5-hour infusions (placebo, iloprost 2 ng/kg/min, PGI2 5 ng/kg/min). Tissue plasminogen activator (t-PA), total plasma fibrinolytic activity and euglobulin clot lysis time (ECLT) were determined in patients before and after each infusion, both in freely flowing blood samples and following 10 min venous occlusion. In patients of group A, ECLT at rest was significantly shortened after all three iloprost infusions (on average by about 5-11%). First and third infusions produced also shortening of ECLT after venostasis (by 21 and 32%). Statistically significant rise in t-PA activity (by about 68% on average) accompanied only the first infusion. In patients of the group B iloprost provoked significant fall in ECLT at rest (by about 19% on average) only. PGI2 shortened ECLT both at rest and after venous occlusion (by about 17% and 20% on average, respectively) and led to a rise in t-PA activity after venous occlusion by about 33% on average. Our results indicate that prostacyclin and its stable analog, iloprost, enhance fibrinolytic activity in man by releasing or facilitating the release of tissue plasminogen activator from the vessel wall.

摘要

我们研究了前列环素(PGI2)及其稳定类似物伊洛前列素对33例外周动脉疾病患者血液纤溶活性的影响。10名受试者(A组)连续三天接受三次为期5小时的伊洛前列素输注。其余23例患者接受三次不同的5小时输注(安慰剂、2 ng/kg/min伊洛前列素、5 ng/kg/min PGI2)。在每次输注前后,对患者自由流动血样以及静脉闭塞10分钟后的组织纤溶酶原激活物(t-PA)、总血浆纤溶活性和优球蛋白凝块溶解时间(ECLT)进行测定。在A组患者中,三次伊洛前列素输注后静息时的ECLT均显著缩短(平均缩短约5 - 11%)。第一次和第三次输注后静脉淤滞时的ECLT也缩短(分别缩短21%和32%)。仅第一次输注伴随t-PA活性有统计学意义的升高(平均升高约68%)。在B组患者中,伊洛前列素仅使静息时的ECLT显著下降(平均下降约19%)。PGI2在静息时和静脉闭塞后均缩短ECLT(平均分别缩短约17%和20%),并使静脉闭塞后t-PA活性平均升高约33%。我们的结果表明,前列环素及其稳定类似物伊洛前列素通过从血管壁释放或促进组织纤溶酶原激活物的释放来增强人体的纤溶活性。

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