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凝血酶作用机制的研究。与纤维蛋白的相互作用。

Studies on the mechanism of thrombin. Interaction with fibrin.

作者信息

Kaminski M, McDonagh J

出版信息

J Biol Chem. 1983 Sep 10;258(17):10530-5.

PMID:6885791
Abstract

Fibrin monomer Sepharose was used to investigate the interactions of thrombin with fibrin. Thrombin binding was found to be reversible and saturable and to depend on the thrombin: fibrin ratio. Scatchard analysis indicated a single class of binding sites with K alpha = 4.9 X 10(5) M-1. Ca2+ ions caused rapid desorption and elution of thrombin from fibrin monomer, and the Ca2+ concentration needed for maximal desorption depended on the fibrin:thrombin ratio. Mg2+, Mn2+, and Sr2+ also released thrombin from fibrin monomer but not as efficiently as Ca2+. These results indicate that divalent metal ions induce a physical change in fibrin monomer which results in desorption of thrombin. Thrombin binding to fibrin in a gel was compared to binding to fibrin monomer. These studies showed that as fibrin monomers polymerize to form the gel network, thrombin is released. Under static conditions the released thrombin remains associated with the gel because diffusion is limited by the gel. However, the thrombin can be readily removed when buffer is allowed to flow through the gel. These results lead to the possibility that thrombin binding to fibrin monomer and its subsequent release, either by Ca2+ or by polymerization, may have important consequences for regulating the effective thrombin concentration in vivo.

摘要

使用纤维蛋白单体琼脂糖来研究凝血酶与纤维蛋白的相互作用。发现凝血酶结合是可逆且可饱和的,并取决于凝血酶与纤维蛋白的比例。Scatchard分析表明存在一类单一的结合位点,解离常数Kα = 4.9×10⁵ M⁻¹。钙离子导致凝血酶从纤维蛋白单体上快速解吸和洗脱,最大解吸所需的钙离子浓度取决于纤维蛋白与凝血酶的比例。镁离子、锰离子和锶离子也能使凝血酶从纤维蛋白单体上释放,但效率不如钙离子。这些结果表明二价金属离子会引起纤维蛋白单体的物理变化,从而导致凝血酶的解吸。将凝胶中凝血酶与纤维蛋白的结合与凝血酶与纤维蛋白单体的结合进行了比较。这些研究表明,随着纤维蛋白单体聚合成凝胶网络,凝血酶会被释放。在静态条件下,释放的凝血酶仍与凝胶结合,因为扩散受到凝胶的限制。然而,当缓冲液流过凝胶时,凝血酶很容易被去除。这些结果提示,凝血酶与纤维蛋白单体的结合及其随后通过钙离子或聚合作用的释放,可能对体内有效凝血酶浓度的调节具有重要意义。

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