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与收缩表型相比,合成型主动脉平滑肌细胞中组织因子和组织因子途径抑制剂的表达上调。

The expression of tissue factor and tissue factor pathway inhibitor in aortic smooth muscle cells is up-regulated in synthetic compared to contractile phenotype.

作者信息

Ghrib Farida, Brisset Anne-Cécile, Dupouy Dominique, Terrisse Anne-Dominique, Navarro Chantal, Cadroy Yves, Boneu Bernard, Sié Pierre

机构信息

EA 2049 Laboratoire de Recherche sur l'Hémostase et la Thrombose, Université Paul Sabatier, Toulouse, France.

出版信息

Thromb Haemost. 2002 Jun;87(6):1051-6.

PMID:12083485
Abstract

Tissue factor (TF) and its specific inhibitor TF pathway inhibitor (TFPI) are produced by vascular smooth muscle cells (SMCs) in vitro and are increased in vivo in atherosclerotic compared to normal vessels. Besides local regulation of the hemostatic balance, this may be related to non-hemostatic TF/protease dependent functions such as SMC proliferation, adhesion and migration. The aim of the study was to compare the expression of both proteins between the contractile (normal adult) and synthetic (neo-intimal) SMC phenotypes. Primary cultures of SMCs isolated from rat thoracic aorta before and 10 days after balloon injury displayed stable characteristics of the contractile and synthetic phenotype, respectively. Synthetic SMCs expressed more TF mRNA than contractile SMCs, but released excess TF in the conditioned medium, so that the cell-associated TF activity measured by a factor Xa generating assay remained similar in the two subtypes. Accordingly, cell surface thrombogenicity measured under blood flow conditions was also similar. The production and release of functional TFPI was enhanced by a factor 3 to 6 (p < 0.01) in synthetic SMCs. A difference in the quantitative expression of TF and TFPI is a new distinctive feature of SMC phenotypes. Matrix-associated TFPI derived from synthetic SMCs may serve as an anchorage for their migration and regulate protease-activated processes during neo-intima formation.

摘要

组织因子(TF)及其特异性抑制剂TF途径抑制剂(TFPI)可由血管平滑肌细胞(SMC)在体外产生,并且与正常血管相比,在动脉粥样硬化血管的体内表达增加。除了对止血平衡的局部调节作用外,这可能还与非止血性的TF/蛋白酶依赖性功能有关,如SMC的增殖、黏附和迁移。本研究的目的是比较收缩型(正常成年)和合成型(新生内膜)SMC表型中这两种蛋白的表达情况。从大鼠胸主动脉分离的SMC原代培养物在球囊损伤前和损伤后10天分别表现出收缩型和合成型表型的稳定特征。合成型SMC比收缩型SMC表达更多的TF mRNA,但在条件培养基中释放出过量的TF,因此通过Xa因子生成试验测定的细胞相关TF活性在两种亚型中保持相似。相应地,在血流条件下测得的细胞表面血栓形成性也相似。合成型SMC中功能性TFPI的产生和释放增加了3至6倍(p<0.01)。TF和TFPI定量表达的差异是SMC表型的一个新的显著特征。源自合成型SMC的基质相关TFPI可能作为其迁移的锚定物,并在新生内膜形成过程中调节蛋白酶激活过程。

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The expression of tissue factor and tissue factor pathway inhibitor in aortic smooth muscle cells is up-regulated in synthetic compared to contractile phenotype.与收缩表型相比,合成型主动脉平滑肌细胞中组织因子和组织因子途径抑制剂的表达上调。
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