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Anti-thrombin activities of heparin. Effect of saccharide chain length on thrombin inhibition by heparin cofactor II and by antithrombin.

机译：肝素的抗凝血酶活性。糖链长度对肝素辅因子II和抗凝血酶抑制凝血酶的影响。

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The interactions of two proteinase inhibitors, heparin cofactor II and antithrombin, with thrombin are potentiated by heparin. Using two methods, we have studied the potentiating effects of a series of heparin (poly)saccharides with high affinity for antithrombin and mean Mr ranging from approx. 1700 to 18,800. First, catalytic amounts of heparin (poly)saccharide were added to purified systems containing thrombin and either heparin cofactor II or antithrombin. Residual thrombin activity was determined with a chromogenic substrate. It was found that only the higher-Mr polysaccharides (Mr greater than 8000) efficiently catalysed thrombin inhibition by heparin cofactor II, there being a progressive catalytic effect with increasing Mr of the polysaccharide. Weak accelerating effects were noted with low-Mr saccharides (Mr less than 8000). This contrasted with the well-characterized interaction of heparin with antithrombin and thrombin, where heparin oligosaccharides of Mr less than 5400 had absolutely no ability to accelerate the reaction, while (poly)saccharides of Mr exceeding 5400 showed rapidly increasing catalytic activity with increasing Mr. Secondly, these and other heparin preparations were added in a wide concentration range to plasma with which 125I-labelled thrombin was then incubated for 30 s. Inhibited thrombin was determined from the distribution of labelled thrombin amongst inhibitor-thrombin complexes, predominantly antithrombin-thrombin and heparin cofactor II-thrombin complexes. In this situation, where the inhibitors competed for thrombin and for the (poly)saccharides, it was found that, provided the latter were of high affinity for antithrombin and exceeded a Mr of 5400, thrombin inhibition in plasma was mediated largely through antithrombin. Polysaccharides of Mr exceeding 8000 that were of low affinity for antithrombin accelerated thrombin inhibition in plasma through their interaction with heparin cofactor II. High concentrations of saccharides of Mr 1700-5400 exhibited a size-dependent acceleration of thrombin inhibition, not through their interaction with antithrombin, but through their interaction with heparin cofactor II.

机译：肝素可增强两种蛋白酶抑制剂，肝素辅因子II和抗凝血酶与凝血酶的相互作用。我们使用两种方法研究了一系列对抗凝血酶具有高亲和力的肝素（多糖）的增强作用，平均Mr范围约为。 1700至18,800。首先，将催化量的肝素（多糖）糖添加到含有凝血酶和肝素辅因子II或抗凝血酶的纯化系统中。用生色底物测定凝血酶的残留活性。发现只有较高Mr的多糖（Mr大于8000）才有效地催化肝素辅因子II对凝血酶的抑制作用，随着多糖Mr的增加，催化作用逐渐增强。低Mr糖（Mr小于8000）观察到微弱的加速作用。这与肝素与抗凝血酶和凝血酶的良好表征的相互作用形成鲜明对比，Mr小于5400的肝素寡糖绝对没有加速反应的能力，而Mr超过5400的（多糖）糖显示出随着Mr增加而迅速增加的催化活性。其次，将这些和其他肝素制剂以宽浓度范围添加到血浆中，然后与125I标记的凝血酶孵育30秒钟。从标记的凝血酶在抑制剂-凝血酶复合物之间的分布确定凝血酶的抑制，主要是抗凝血酶-凝血酶和肝素辅因子II-凝血酶复合物。在这种情况下，在抑制剂竞争凝血酶和（多糖）糖的情况下，发现只要后者对抗凝血酶具有高亲和力并超过5400的Mr，血浆中对凝血酶的抑制作用很大程度上是由抗凝血酶介导的。对抗凝血酶低亲和力的Mr超过8000的多糖通过与肝素辅因子II的相互作用而加速了血浆中对凝血酶的抑制作用。 Mr 1700-5400的高浓度糖类不依赖于与抗凝血酶的相互作用，而是与肝素辅因子II的相互作用，表现出对凝血酶抑制作用的大小依赖性加速作用。

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Bray, B; Lane, D A; Freyssinet, J M; Pejler, G; Lindahl, U;
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年度 1989
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1. Anti-thrombin activities of heparin. Effect of saccharide chain length on thrombin inhibition by heparin cofactor II and by antithrombin [J] . B Bray, D A Lane, G Pejler, The biochemical journal . 1989,第1期

机译：肝素的抗凝血酶活性。糖链长度对肝素辅因子II和抗凝血酶抑制凝血酶的影响
2. Low molecular weight heparins prevent thrombin-induced thrombo-embolism in mice despite low anti-thrombin activity. Evidence that the inhibition of feed-back activation of thrombin generation confers safety advantages over direct thrombin inhibition | Haematologica [J] . S Momi, M Nasimi, M Colucci, Haematologica . 2001,第3期

机译：尽管抗凝血酶活性较低，但低分子量肝素仍可预防小鼠凝血酶诱导的血栓栓塞。与直接抑制凝血酶相比，抑制凝血酶产生的反馈激活具有安全优势的证据血液学
3. Binding of heparin or dermatan sulfate to thrombin is essential for the sulfated polysaccharide‐accelerated inhibition of thrombin by heparin cofactor II [J] . Koide Takehiko, Sakuragawa Nobuo, Yamagishi Ryoichi FEBS Letters . 1987,第1a2期

机译：肝素或硫酸皮肤素与凝血酶的结合对于肝素辅因子II对硫酸化多糖加速凝血酶的抑制至关重要
4. Probing interactions of different glycoforms of antithrombin- III with heparin octa-/deca-saccharides using native electrospray ionization mass spectrometry [C] . Rinat R. Abzalimov, Burcu B. Minsky, Stephen J. Eyles, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2013

机译：用天然电喷雾电离质谱法探测抗凝血酶-III与肝素Octa-/ Deca-糖的不同糖族的相互作用
5. I. Comparison of translesion bypass of guanine-N2 monoadducts of mitomycin C and guanine -N7 monoadducts of 2,7-diaminomitosene by T7 exo-, Klenow exo-, eta and Klenow exo+ DNA polymerases. II. Structure-based design, synthesis, structure-conformation and structure -activity relationships studies of D-Phe-Pro-D-Arg-P1'-CONH2 tetrapeptides with inhibitory activity for thrombin. [D] . Clement, Cristina C. 2006

机译：I.通过T7 exo-，Klenow exo-，eta和Klenow exo + DNA聚合酶比较丝裂霉素C的鸟嘌呤-N2单加合物和2,7-二氨基光油的鸟嘌呤-N7单加合物的跨病变旁路。二。具有凝血酶抑制活性的D-Phe-Pro-D-Arg-P1'-CONH2四肽的基于结构的设计，合成，结构构象和结构-活性关系研究。
6. Anti-thrombin activities of heparin. Effect of saccharide chain length on thrombin inhibition by heparin cofactor II and by antithrombin. [O] . B Bray, D A Lane, J M Freyssinet, 1989

机译：肝素的抗凝血酶活性。糖链长度对肝素辅因子II和抗凝血酶抑制凝血酶的影响。
7. Structure-activity relationships of heparin. Independence of heparin charge density and antithrombin-binding domains in thrombin inhibition by antithrombin and heparin cofactor II. [O] . Hurst, R E, Poon, M C, Griffith, M J 1983

机译：肝素的构效关系。肝素电荷密度和抗凝血酶结合域在抗凝血酶和肝素辅因子II抑制凝血酶方面的独立性。

Anti-thrombin activities of heparin. Effect of saccharide chain length on thrombin inhibition by heparin cofactor II and by antithrombin.

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