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首页> 外文期刊>Antioxidants and redox signalling >Extracellular disulfide exchange and the regulation of cellular function.
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Extracellular disulfide exchange and the regulation of cellular function.

机译:细胞外二硫键交换和细胞功能的调节。

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摘要

An emerging concept is that disulfide bonds can act as a dynamic scaffold to present mature proteins in different conformational and functional states on the cell surface. Two examples are the conversion of the receptor, integrin alphaIIbbeta3, from a low affinity to a high affinity state, and the interaction of CD4 receptor with the HIV-1 envelope glycoprotein gp120 to promote virus-cell fusion. In both of these cases there is a remodeling of the protein disulfide bonding pattern. The formation and rearrangement of disulfide bonds is modulated by a family of enzymes known as the thiol isomerases, which include protein disulfide isomerase (PDI), ERp5, ERp57, and ERp72. While these enzymes were reported originally to be restricted in location to the endoplasmic reticulum, in some cells thiol isomerases are found on the cell surface. This may indicate a wider role for these enzymes in cell function. In platelets it has been shown that reagents that react with cell surface sulfhydryl groups are capable of blocking a number of functional responses, including integrin-mediated aggregation, adhesion, and granule secretion. Furthermore, the use of function blocking antibodies to either PDI or ERp5 causes inhibition of these functional responses. This review summarizes current knowledge of the extracellular regulation of disulfide exchange and the implications of this in the regulation of cell function.
机译:一个新兴的概念是二硫键可以充当动态支架,以在细胞表面呈现不同构象和功能状态的成熟蛋白质。两个例子是受体整合素αIIbbeta3从低亲和力状态转变为高亲和力状态,以及CD4受体与HIV-1包膜糖蛋白gp120相互作用以促进病毒-细胞融合。在这两种情况下,都存在蛋白质二硫键结合模式的重塑。二硫键的形成和重排受称为硫醇异构酶的酶家族调节,这些酶包括蛋白质二硫键异构酶(PDI),ERp5,ERp57和ERp72。尽管最初报道这些酶局限于内质网,但在某些细胞的表面发现了巯基异构酶。这可能表明这些酶在细胞功能中具有更广泛的作用。在血小板中,已经表明与细胞表面巯基反应的试剂能够阻断多种功能反应,包括整联蛋白介导的聚集,粘附和颗粒分泌。此外,使用针对PDI或ERp5的功能阻断抗体会抑制这些功能反应。这篇综述总结了目前关于二硫键交换的细胞外调节的知识,以及其对细胞功能调节的影响。

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