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功能性组织因子在脂多糖刺激的人血单核细胞和组成型产生组织因子的肿瘤细胞系上完全表达于细胞表面。

Functional tissue factor is entirely cell surface expressed on lipopolysaccharide-stimulated human blood monocytes and a constitutively tissue factor-producing neoplastic cell line.

作者信息

Drake T A, Ruf W, Morrissey J H, Edgington T S

机构信息

Department of Pathology, University of California, Los Angeles 90024-1732.

出版信息

J Cell Biol. 1989 Jul;109(1):389-95. doi: 10.1083/jcb.109.1.389.

Abstract

Tissue factor (TF) is an integral membrane glycoprotein which, as the receptor and essential cofactor for coagulation factors VII and VIIa (FVII and FVIIa, respectively), is the primary cellular activator of the coagulation protease cascade. Previous studies on the procoagulant activity of a variety of cell types (either lysed or in the intact state) have variously been interpreted as showing that TF is either stored intracellularly or is present in a cryptic form in the surface membrane. Using mAbs to TF, we have directly investigated the subcellular localization and functional activity of TF in lipopolysaccharide-stimulated blood monocytes and J82 bladder carcinoma cells. Blocking of surface TF of viable cells with inhibitory anti-TF mAbs abolished greater than 90% of TF activity of the intact cells as well as of lysed cells. Furthermore, quantitative analysis of the binding of FVII and anti-TF mAb to J82 cells demonstrated that all surface-expressed TF molecules were capable of binding the ligand, FVII. By immunoelectron microscopy, TF was present only in the surface membrane of monocytes and J82 cells, although the latter also contained apparently inactive TF antigen in multivesicular bodies. On the intact cell surface the catalytic activity of the TF-FVIIa complex was investigated and found to be markedly less relative to cell lysates. Membrane alterations that affect the cofactor activity of TF may be a means of regulating the extent of initiation of the coagulation protease cascade in various cellular settings.

摘要

组织因子(TF)是一种整合膜糖蛋白,作为凝血因子VII和VIIa(分别为FVII和FVIIa)的受体和必需辅因子,是凝血蛋白酶级联反应的主要细胞激活剂。先前对多种细胞类型(裂解或完整状态)促凝活性的研究,其结果被不同地解释为表明TF要么储存在细胞内,要么以隐蔽形式存在于表面膜中。我们使用针对TF的单克隆抗体,直接研究了脂多糖刺激的血液单核细胞和J82膀胱癌细胞中TF的亚细胞定位和功能活性。用抑制性抗TF单克隆抗体阻断活细胞的表面TF,可消除完整细胞以及裂解细胞中90%以上的TF活性。此外,对FVII和抗TF单克隆抗体与J82细胞结合的定量分析表明,所有表面表达的TF分子都能够结合配体FVII。通过免疫电子显微镜观察,TF仅存在于单核细胞和J82细胞的表面膜中,尽管后者的多泡体中也含有明显无活性的TF抗原。在完整细胞表面研究了TF-FVIIa复合物的催化活性,发现其相对于细胞裂解物明显较低。影响TF辅因子活性的膜改变可能是在各种细胞环境中调节凝血蛋白酶级联反应起始程度的一种方式。

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