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重组组织因子途径抑制剂增强因子Xa与人单核细胞的结合。

Recombinant tissue factor pathway inhibitor enhances the binding of factor Xa to human monocytes.

作者信息

Li A, Chang A C, Peer G T, Wun T C, Taylor F B

机构信息

Cardiovascular Biology Program, Oklahoma Medical Research Foundation, Oklahoma City 73104, USA.

出版信息

Thromb Haemost. 2001 May;85(5):830-6.

Abstract

Tissue factor pathway inhibitor (TFPI) is a kunitz-type inhibitor of activated factor X (Xa). TFPI was reported to mediate Xa binding to a few of carcinoma cell lines. In this study it was observed that the Xa activity associated with human peripheral blood mononuclear cells (PBMC) incubated with Xa in the presence of recombinant TFPI (rTFPI) was much higher than with Xa alone. Xa activity on PBMC was also observed after whole blood was incubated with pre-formed Xa/TFPI complex. Further studies with flow cytometric analysis demonstrate that rTFPI enhances the binding of Xa to human monocytes. Western blot analysis showed that rTFPI was cleaved into a few of fragments after its incubation with monocytes either in the presence or absence of Xa. Based on these results and the observations reported by others, we speculate that Xa/TFPI complex may bind to human monocytes by a yet unidentified mechanism. The recovery of Xa activity from Xa/TFPI complex on PBMC may be related to the cleavage of rTFPI by Xa and/or monocyte proteases. This observation suggests a new mechanism by which monocytes become procoagulant in some pathological conditions in addition of the well known tissue factor expression on proinflammatic monocytes.

摘要

组织因子途径抑制剂(TFPI)是一种库尼茨型活化因子X(Xa)抑制剂。据报道,TFPI可介导Xa与一些癌细胞系结合。在本研究中,观察到在重组TFPI(rTFPI)存在的情况下,与Xa孵育的人外周血单个核细胞(PBMC)相关的Xa活性远高于单独使用Xa时。在用预先形成的Xa/TFPI复合物孵育全血后,也观察到了PBMC上的Xa活性。流式细胞术分析的进一步研究表明,rTFPI增强了Xa与人单核细胞的结合。蛋白质印迹分析表明,rTFPI在与单核细胞孵育后,无论有无Xa,都会被切割成几个片段。基于这些结果以及其他人的观察,我们推测Xa/TFPI复合物可能通过一种尚未明确的机制与人单核细胞结合。PBMC上Xa/TFPI复合物中Xa活性的恢复可能与Xa和/或单核细胞蛋白酶对rTFPI的切割有关。这一观察结果提示了一种新的机制,除了众所周知的促炎单核细胞上组织因子的表达外,单核细胞在某些病理条件下可成为促凝细胞。

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