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首页> 外文期刊>Thrombosis and Haemostasis: Journal of the International Society on Thrombosis and Haemostasis >Effects of heparin and related sulfated polysaccharides on tissue factor expression induced by mitogenic and non-mitogenic factors in human vascular smooth muscle cells.
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Effects of heparin and related sulfated polysaccharides on tissue factor expression induced by mitogenic and non-mitogenic factors in human vascular smooth muscle cells.

机译:肝素和相关硫酸化多糖对人血管平滑肌细胞中有丝分裂和非有丝分裂因子诱导的组织因子表达的影响。

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摘要

Smooth muscle cells (SMCs) of the intima are generally quiescent and non proliferative. Their proliferation due to different stimulations occurs in myointimal hyperplasia and is regularly present in atherogenesis or after transluminal angioplasty leading to vascular occlusive stenosis. In the course of these pathologies, the Tissue Factor (TF) synthesis was upregulated and rapidly expressed at the membrane of the SMCs. Heparin is known to inhibit SMCs proliferation induced by FCS. We evaluated the inhibitory effect of heparin on the expression of TF induced by various mitogenic (FCS, PDGF-BB and EGF) and non-mitogenic (bacterial LPS) agents. Inhibition by heparin of SMCs proliferation induced by the same agonists was also determined. Quiescent human vascular SMCs from normal adult arteries were treated for 1 h by heparin and related sulfated polysaccharides before stimulation by the agonists. All the agonists up-regulated the expression of TF antigen and activity. TF expression induced by the growth factors was inhibited by heparin (IC 50: 10-30 microg/ml), and other sulfated polysaccharides (IC 50: 1-5 microg/ml). SMCs proliferation, late activation of the extracellular signal-regulated kinases (ERK1/2), and PKC activity were inhibited by heparin (IC 50: 30-50 microg/ml) in SMCs stimulated by FCS but not in SMCs treated by PDGF or EGF. In contrast, heparin had no effect on LPS-induced TF expression nor on LPS-induced PKC activation. These results indicate that, besides its well known effect on SMC proliferation, heparin displays an inhibitory effect on cell mediated blood clotting processes through regulation of the TF expression.
机译:内膜的平滑肌细胞(SMCs)通常是静止的且不增殖。由于不同的刺激,它们的增殖发生在肌内膜增生中,并经常存在于动脉粥样硬化或腔内血管成形术后,导致血管闭塞性狭窄。在这些病理过程中,组织因子(TF)的合成被上调并在SMC膜上迅速表达。已知肝素可抑制FCS诱导的SMC增殖。我们评估了肝素对各种有丝分裂剂(FCS,PDGF-BB和EGF)和非有丝分裂剂(细菌LPS)诱导的TF表达的抑制作用。还确定了肝素对相同激动剂诱导的SMCs增殖的抑制。在激动剂刺激之前,用肝素和相关的硫酸化多糖处理正常成人动脉的静态人血管SMC 1小时。所有的激动剂均上调了TF抗原的表达和活性。肝素(IC 50:10-30微克/毫升)和其他硫酸化多糖(IC 50:1-5微克/毫升)抑制了生长因子诱导的TF表达。在FCS刺激的SMC中,肝素(IC 50:30-50 microg / ml)抑制SMCs增殖,细胞外信号调节激酶(ERK1 / 2)的晚期激活和PKC活性,但在PDGF或EGF处理的SMC中则不抑制SMCs 。相反,肝素对LPS诱导的TF表达或LPS诱导的PKC活化均无影响。这些结果表明,除了众所周知的对SMC增殖的作用外,肝素还通过调节TF表达对细胞介导的凝血过程显示出抑制作用。

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