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Kinetics of factor Xa inhibition by tissue factor pathway inhibitor.

作者信息

Huang Z F, Wun T C, Broze G J

机构信息

Division of Hematology/Oncology, Jewish Hospital, Washington University Medical Center, St. Louis, Missouri 63110.

出版信息

J Biol Chem. 1993 Dec 25;268(36):26950-5.

PMID:8262929
Abstract

Tissue factor pathway inhibitor is a multivalent, Kunitz-type proteinase inhibitor. It directly inhibits factor Xa and, in a factor Xa-dependent fashion, produces feedback inhibition of the factor VIIa/tissue factor catalytic complex which is responsible for the initiation of coagulation. Human recombinant TFPI (rTFPI) produced in Escherichia coli was used to define the kinetic constants describing the human factor Xa:TFPI interaction. The inactivation of factor Xa by E. coli-rTFPI is indistinguishable from that of rTFPI produced in mammalian SK-hepatoma cells, suggesting that post-translational modifications such as glycosylation and phosphorylation do not play a major role in the inhibitory process. The slow, tight-binding inhibition of factor Xa follows the scheme: [formula: see text] Where the enzyme (E) and inhibitor (I) form an initial, immediate collision complex (EI) that then isomerizes slowly to a tightened final EI* complex. In the absence of other additions, the initial Ki (=k2/k1) and final Ki* for the inhibition of factor Xa by E. coli-rTFPI are 1.24 nM and 26.4 pM, respectively. In the presence of calcium ions (5 mM) the interaction between factor Xa and rTFPI is substantially weaker, with a Ki of 42.7 nM and Ki* of 85.2 pM. The addition of other components of the prothrombinase complex produces enhanced factor Xa inhibition predominantly through an effect on the initial Ki. In the presence of calcium ions and saturating concentrations of phospholipids and factor Va, the Ki and Ki* for factor Xa inactivation are 2.04 nM and 52.3 pM. The enhancing effect of heparin on the inhibitory process is concentration dependent and exhibits an optimum, reminiscent of the "template" model for heparin's acceleration of thrombin and factor IXa inhibition by antithrombin III. At optimal concentrations, the major mechanism of heparin action is also a reduction in the Ki of the initial encounter complex between factor Xa and rTFPI.

摘要

相似文献

1
Kinetics of factor Xa inhibition by tissue factor pathway inhibitor.
J Biol Chem. 1993 Dec 25;268(36):26950-5.
2
Tissue factor pathway inhibitor: the carboxy-terminus is required for optimal inhibition of factor Xa.组织因子途径抑制物:对因子Xa的最佳抑制作用需要羧基末端。
Blood. 1992 Apr 15;79(8):2004-10.
3
Effect of heparin on the inhibition of factor Xa by tissue factor pathway inhibitor: a segment, Gly212-Phe243, of the third Kunitz domain is a heparin-binding site.肝素对组织因子途径抑制剂抑制因子Xa的影响:第三个Kunitz结构域的一段,即Gly212 - Phe243,是一个肝素结合位点。
Biochemistry. 1995 May 2;34(17):5725-35. doi: 10.1021/bi00017a004.
4
Structural requirements for tissue factor pathway inhibitor interactions with factor Xa and heparin.组织因子途径抑制剂与因子Xa及肝素相互作用的结构要求
Blood Coagul Fibrinolysis. 1993 Oct;4(5):661-9.
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Kinetics of the inhibition of factor Xa and the tissue factor-factor VIIa complex by the tissue factor pathway inhibitor in the presence and absence of heparin.组织因子途径抑制物在存在和不存在肝素的情况下对因子Xa及组织因子-因子VIIa复合物的抑制动力学
Biochemistry. 1994 Oct 25;33(42):12686-94. doi: 10.1021/bi00208a020.
6
Physiological concentrations of tissue factor pathway inhibitor do not inhibit prothrombinase.
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7
The effect of leukocyte elastase on tissue factor pathway inhibitor.白细胞弹性蛋白酶对组织因子途径抑制物的作用。
Blood. 1992 Apr 1;79(7):1712-9.
8
A kinetic analysis of the interaction of human recombinant tissue factor pathway inhibitor with factor Xa utilizing and immunoassay and the effect of antithrombin III/heparin on the complex formation.利用免疫测定法对重组人组织因子途径抑制物与因子Xa相互作用的动力学分析以及抗凝血酶III/肝素对复合物形成的影响。
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Eur J Biochem. 1996 Jan 15;235(1-2):310-6. doi: 10.1111/j.1432-1033.1996.0310f.x.

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