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全血中“自发性”血小板聚集的抑制剂。

Inhibitors of "spontaneous" platelet aggregation in whole blood.

作者信息

Harrison M J, Pollock S S, Steiner M, Weisblatt E

出版信息

Atherosclerosis. 1985 Dec;58(1-3):199-203. doi: 10.1016/0021-9150(85)90066-8.

Abstract

In vitro 'spontaneous' platelet aggregation has been studied in whole blood. The spectrum of activity of materials known to influence platelet aggregation in platelet-rich plasma proved different in whole blood. Thus dipyridamole and one of its analogues SH1242 had a striking effect in whole blood whilst aspirin, chlorpromazine and K3920 had little or no effect. The combination of aspirin and dipyridamole as currently employed in clinical practice had no greater inhibitory effect than dipyridamole alone. The possible clinical relevance of these findings is discussed.

摘要

已对全血中的体外“自发性”血小板聚集进行了研究。已知影响富血小板血浆中血小板聚集的物质的活性谱在全血中有所不同。因此,双嘧达莫及其类似物之一SH1242在全血中具有显著作用,而阿司匹林、氯丙嗪和K3920几乎没有作用或根本没有作用。临床实践中目前使用的阿司匹林和双嘧达莫组合的抑制作用并不比单独使用双嘧达莫更大。讨论了这些发现可能的临床相关性。

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