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[血小板类前列腺素及致密颗粒分泌产物在血小板于胶原底物上的黏附、铺展和聚集过程中的作用]

[The role of thrombocyte prostanoids and products secreted by dense granules in the platelet attachment, spreading and aggregation on collagen substrates].

作者信息

Leĭtin V L, Missel'vits F, Liubimova E V, Domogatskiĭ S P

出版信息

Biokhimiia. 1989 Nov;54(11):1804-14.

PMID:2516746
Abstract

The role of platelet prostanoids and substances released from dense bodies (ADP and serotonin) in the initial attachment, spreading and aggregation of platelets on surfaces coated with I, III, IV and V genetic types of collagen was investigated. A positive linear correlation was found to exist between thrombi-like aggregate formation on collagen substrates and platelet prostanoid synthesis. No correlation was established between platelet aggregate formation and 14C-serotonin release. The cyclooxygenase inhibitor indomethacin and the antagonists of PG endoperoxides and TXA2 (13-APA and BM 13.177) completely block thrombi-like aggregate formation. Neither 13-APA nor BM 13.177 affect platelet spreading, while indomethacin inhibits this process by 25%. The ADP-scavenger CP/CPK inhibits platelet aggregation and spreading by 25-30%. The inhibitors of cyclooxygenase and CP/CPK do not influence the initial attachment of platelets. The data obtained suggest that thrombi-like aggregate formation on collagen substrates is mediated by the synthesis of PG endoperoxides and TXA2; however, in platelet spreading this synthesis plays a limited role. Spreading and aggregation of platelets on collagen substrates is only partly mediated by ADP and serotonin. Initial attachment of platelets does not depend on ADP and serotonin release and PG endoperoxide/TXA2 synthesis.

摘要

研究了血小板类前列腺素以及致密体释放的物质(ADP和血清素)在血小板于涂有I、III、IV和V型胶原的表面上的初始黏附、铺展和聚集过程中的作用。结果发现,在胶原底物上形成血栓样聚集体与血小板类前列腺素合成之间存在正线性相关。血小板聚集体形成与14C-血清素释放之间未建立相关性。环氧化酶抑制剂吲哚美辛以及PG内过氧化物和TXA2的拮抗剂(13-APA和BM 13.177)完全阻断血栓样聚集体的形成。13-APA和BM 13.177均不影响血小板铺展,而吲哚美辛可使该过程受到25%的抑制。ADP清除剂CP/CPK可使血小板聚集和铺展受到25% - 30%的抑制。环氧化酶抑制剂和CP/CPK不影响血小板的初始黏附。所获得的数据表明,在胶原底物上形成血栓样聚集体是由PG内过氧化物和TXA2的合成介导的;然而,在血小板铺展过程中,这种合成作用有限。血小板在胶原底物上的铺展和聚集仅部分由ADP和血清素介导。血小板的初始黏附不依赖于ADP和血清素的释放以及PG内过氧化物/TXA2的合成。

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