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一种新型前列环素类似物ZK36374对人全血中血小板聚集的新作用。

The novel effect of a new prostacyclin analogue ZK36374 on the aggregation of human platelets in whole blood.

作者信息

Saniabadi A R, Lowe G D, Belch J J, Forbes C D, Prentice C R, Barbenel J C

出版信息

Thromb Haemost. 1983 Oct 31;50(3):718-21.

PMID:6196854
Abstract

Platelet aggregation was studied at 37 degrees C in citrated whole human blood, using the Ultra Flo 100 Whole Blood Platelet Counter. Aggregation was measured as a fall in the number of single platelets following addition of an aggregating agent. At peak aggregation, the fall in the number of platelets induced by ADP (10 microM), collagen (1 microgram/ml) or thrombin (0.2 U/ml) was about 90%. When blood was incubated with the prostacyclin-analogue ZK36374, the aggregation responses to ADP, collagen and thrombin were reduced with IC50's = 0.5, 1.5 and 3 nM respectively and the corresponding IC100's were: 1, 3 and 12 nM. When ZK36374 was added at peak aggregation, the number of single platelets increased significantly due to disaggregation of preformed platelet aggregates. It is concluded that the present technique represents a rapid, sensitive and more physiological approach for investigating the effects of pharmacological agents on platelet aggregation.

摘要

使用Ultra Flo 100全血血小板计数器,在37摄氏度下对枸橼酸化的全人血中的血小板聚集进行了研究。聚集通过添加聚集剂后单个血小板数量的下降来测量。在聚集峰值时,由ADP(10微摩尔)、胶原蛋白(1微克/毫升)或凝血酶(0.2单位/毫升)诱导的血小板数量下降约90%。当血液与前列环素类似物ZK36374孵育时,对ADP、胶原蛋白和凝血酶的聚集反应分别降低,IC50分别为0.5、1.5和3纳摩尔,相应的IC100分别为:1、3和12纳摩尔。当在聚集峰值时添加ZK36374时,由于预先形成的血小板聚集体的解聚,单个血小板的数量显著增加。得出的结论是,本技术是一种快速、灵敏且更符合生理的方法,用于研究药理剂对血小板聚集的影响。

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