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首页> 外文期刊>Life sciences >Involvement of a calcium-independent pathway in plasmin-induced platelet shape change.
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Involvement of a calcium-independent pathway in plasmin-induced platelet shape change.

机译:钙独立途径参与纤溶酶诱导的血小板形状改变。

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Plasmin-induced platelet activation is considered to be a cause of reocclusion after thrombolytic therapy with plasminogen activators. However, little is known regarding its mechanism and regulation, particularly with respect to the initial step shape change. We here demonstrate that a Ca2+-independent pathway is involved in plasmin-induced human platelet shape change, and that Rho-kinase plays an important role in this pathway. When the increase in cytosolic Ca2+ was prevented by an intracellular Ca2+ chelator, 5,5'-dimethyl-BAPTA, plasmin-induced platelet shape change was partially inhibited but still occurred. In the presence of 5,5'-dimethyl-BAPTA, a specific Rho-kinase inhibitor, Y-27632, completely inhibited the shape change. Phosphorylation of myosin light chain, a key regulator of platelet shape change, was completely inhibited by Y-27632 in 5,5'-dimethyl-BAPTA-treated platelets. Although plasmin caused tyrosine phosphorylation of the 80 kDa protein during the shape change, it did not seem to have a critical role. cAMP-elevating agents inhibited plasmin-induced shape change in 5,5'-dimethyl-BAPTA- or Y-27632-treated platelets with similar efficiency. These results indicated that plasmin causes platelet shape change by activating Ca2+-dependent and Ca2+-independent-Rho-kinase-dependent pathways, both of which are sensitive to cAMP.
机译:用纤溶酶原激活剂进行溶栓治疗后,血浆纤溶酶诱导的血小板活化被认为是重新闭塞的原因。然而,关于其机理和调节,特别是关于初始台阶形状变化的了解很少。我们在这里证明,Ca2 +依赖性途径参与纤溶酶诱导的人类血小板形状变化,并且Rho激酶在该途径中起重要作用。当胞内Ca2 +螯合剂5,5'-二甲基-BAPTA阻止了胞浆Ca2 +的增加时,纤溶酶诱导的血小板形状改变被部分抑制,但仍然发生。在5,5'-二甲基-BAPTA存在下,特定的Rho激酶抑制剂Y-27632完全抑制了形状变化。 Y-27632在5,5'-二甲基-BAPTA处理的血小板中完全抑制了肌球蛋白轻链的磷酸化(血小板形状变化的关键调节剂)。尽管纤溶酶在形状变化过程中引起80 kDa蛋白的酪氨酸磷酸化,但似乎没有关键作用。在5,5'-二甲基-BAPTA或Y-27632处理的血小板中,cAMP增强剂抑制了纤溶酶诱导的形状变化,效率相似。这些结果表明纤溶酶通过激活依赖于cAMP的Ca2 +依赖性和Ca2 +依赖性Rho激酶依赖性途径来引起血小板形状改变。

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