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合成直接凝血酶拮抗剂作用机制研究中的方法学问题

Methodological aspects in the studies on the mechanism of action of synthetic direct thrombin antagonists.

作者信息

Bagdy D, Barabás E, Szabó G

机构信息

Institute for Drug Research Ltd., Budapest, Hungary.

出版信息

Acta Physiol Hung. 1994;82(4):355-63.

PMID:7785446
Abstract

Requirements reported for an ideal anticoagulant [12] and for an ideal antithrombotic [18] show the necessity of many-sided methodological approach in order to detect the molecular mechanism of action of a novel synthetic antagonist of thrombin. The lack of a protocol internationally accepted, on the one hand, and with regard to a general proposal accepted [16], on the other hand, authors applied a complex methodological system involving also the study on the possible interactions at molecular level of some novel thrombin antagonists with the main components of their site of action. The surprising contradiction found between in vitro and in vivo efficacy of several antagonists could be attributed and explained by the significant differences in Ki and IC50 values determined in complex clotting assays containing plasma proteins and/or blood cells versus those measured in reaction mixtures consisting of a synthetic chromogenic substrate, the target enzyme, thrombin, and the antagonist compound in buffer solution.

摘要

对于理想抗凝剂[12]和理想抗血栓药物[18]所报道的要求表明,为了检测新型凝血酶合成拮抗剂的分子作用机制,需要采用多方面的方法。一方面缺乏国际公认的方案,另一方面就已接受的总体提议而言[16],作者应用了一个复杂的方法体系,其中还包括研究一些新型凝血酶拮抗剂在分子水平上与其作用位点主要成分之间可能的相互作用。几种拮抗剂在体外和体内疗效之间发现的惊人矛盾,可以归因于并解释为在含有血浆蛋白和/或血细胞的复杂凝血试验中测定的Ki和IC50值,与在由合成显色底物、靶酶凝血酶和缓冲溶液中的拮抗剂化合物组成的反应混合物中测得的值存在显著差异。

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