[Regulation of thrombocyte stimulating and other activities of thrombin by modulators of the recognition site].

S M Strukova, T N Dugina, E G Kireeva, L I Brodskiĭ, A E Kogan, I P Ashmarin
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引用次数: 0

Abstract

The structural and functional features of thrombin are under discussion: combination of restricted specificity and a central regulatory role in hemostasis. Thrombin specificity is mainly connected with special regions of the enzyme molecule--an additional recognition binding site for high molecular substrates. One can consider the additional site of thrombin as a kind of the allosteric centre changing thrombin-catalyzed functions at binding with modulator. Specific site of substrate (inhibitor or receptor) is used in the role of modulator. A computer search of that modulator was fulfilled by means of the program DOTHELIX. The peptides thymosin I and substance P which have regions similar to those of hirudin were shown to inhibit thrombin activity. The kinetic data point to the noncompetitive type of inhibition. The data on the high reactivity of the thrombin-activated protein C system confirm the idea of protein C to be the first defensive mechanism when thrombin is generated in blood and interacts with thrombomodulin.

[识别位点调节剂对促血小板及其他凝血酶活性的调节]。
凝血酶的结构和功能特征正在讨论中:限制特异性和止血中心调节作用的结合。凝血酶的特异性主要与酶分子的特殊区域有关,这是对高分子底物的额外识别结合位点。我们可以把凝血酶的附加位点看作是一种改变凝血酶与调节剂结合时的变构中心。底物(抑制剂或受体)的特定位点起调制剂的作用。利用dotheelix程序对该调制器进行了计算机搜索。胸腺肽I和P物质具有与水蛭素相似的区域,可抑制凝血酶活性。动力学数据指向非竞争性抑制类型。关于凝血酶激活蛋白C系统的高反应性的数据证实了当凝血酶在血液中产生并与血栓调节蛋白相互作用时,蛋白C是第一个防御机制的观点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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