Analysis of endothelial protein C receptor functionality on living cells'.

Q3 Biochemistry, Genetics and Molecular Biology
E Ducros, S Mirshahi, C Bermot, M Mirshahi
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引用次数: 0

Abstract

Activated protein C (APC) is a major control system of blood coagulation. APC prevents coagulation pathway by degrading Va and VIIIa plasma's coagulation factors. Protein C activation requires its binding to specific endothelial cell receptor (EPCR). APC binding to EPCR also activates a wide range of defense mechanisms (anti-inflammatory, antiapoptosis...). EPCR expression by cells can be detected by various methods, including immunoanalysis and molecular biology. However, no assays evaluate its functionality. A method, inspired of a standard fibrinoformation time assay, was developed to estimate EPCR ability to bind APC on living cell surface in vitro. Endothelial cells were incubated with APC and fibrinoformation on cells was followed by spectrophotometry (plasma absorbance increases with fibrin polymerization). Membrane-bound EPCR retain APC, thus prolonging fibrinoformation time in a dose-dependent manner. Control was realized with EPCR-negative cells. This new method can be used on any cell type to study the expression of other coagulation receptors.

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内皮蛋白C受体在活细胞上的功能分析
活化蛋白C (Activated protein C, APC)是血液凝固的主要控制系统。APC通过降解Va和viia血浆的凝血因子阻止凝血途径。蛋白C的激活需要与特定的内皮细胞受体(EPCR)结合。与EPCR结合的APC还可激活多种防御机制(抗炎、抗凋亡等)。EPCR在细胞中的表达可以通过多种方法检测,包括免疫分析和分子生物学。然而,没有分析评估其功能。受标准纤维信息形成时间测定的启发,开发了一种方法来估计EPCR在体外活细胞表面结合APC的能力。内皮细胞用APC孵育,用分光光度法观察细胞的纤维信息形成(血浆吸光度随纤维蛋白聚合而增加)。膜结合EPCR保留APC,从而以剂量依赖的方式延长纤维信息形成时间。用epcr阴性细胞进行对照。这种新方法可用于任何细胞类型来研究其他凝血受体的表达。
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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来源期刊
Open Biochemistry Journal
Open Biochemistry Journal Biochemistry, Genetics and Molecular Biology-Biochemistry, Genetics and Molecular Biology (all)
CiteScore
1.50
自引率
0.00%
发文量
5
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