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首页> 外文期刊>Cell death & disease. >Impairment of Fas-ligand–caveolin-1 interaction inhibits Fas-ligand translocation to rafts and Fas-ligand-induced cell death
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Impairment of Fas-ligand–caveolin-1 interaction inhibits Fas-ligand translocation to rafts and Fas-ligand-induced cell death

机译:Fas-配体-caveolin-1相互作用的障碍抑制了Fas-配体向木筏的转运和Fas-配体诱导的细胞死亡。

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Fas-ligand/CD178 belongs to the TNF family proteins and can induce apoptosis through death receptor Fas/CD95. The important requirement for Fas-ligand-dependent cell death induction is its localization to rafts, cholesterol- and sphingolipid-enriched micro-domains of membrane, involved in regulation of different signaling complexes. Here, we demonstrate that Fas-ligand physically associates with caveolin-1, the main protein component of rafts. Experiments with cells overexpressing Fas-ligand revealed a FasL N-terminal pre-prolin-rich region, which is essential for the association with caveolin-1. We found that the N-terminal domain of Fas-ligand bears two caveolin-binding sites. The first caveolin-binding site binds the N-terminal domain of caveolin-1, whereas the second one appears to interact with the C-terminal domain of caveolin-1. The deletion of both caveolin-binding sites in Fas-ligand impairs its distribution between cellular membranes, and attenuates a Fas-ligand-induced cytotoxicity. These results demonstrate that the interaction of Fas-ligand and caveolin-1 represents a molecular basis for Fas-ligand translocation to rafts, and the subsequent induction of Fas-ligand-dependent cell death. A possibility of a similar association between other TNF family members and caveolin-1 is discussed.
机译:Fas-配体/ CD178属于TNF家族蛋白,可通过死亡受体Fas / CD95诱导凋亡。 Fas-配体依赖性细胞死亡诱导的重要要求是其定位于筏,富含胆固醇和鞘脂的膜微区,参与调节不同的信号复合物。在这里,我们证明Fas-配体与小筏的主要蛋白质组分Caveolin-1物理结合。使用过表达Fas-配体的细胞进行的实验表明,FasL N端富含前脯氨酸的区域对于与Caveolin-1的结合至关重要。我们发现,Fas-配体的N-末端结构域带有两个小窝蛋白结合位点。第一个小窝蛋白结合位点与小窝蛋白1的N末端域结合,而第二个小窝结合位点似乎与小窝蛋白1的C末端域相互作用。 Fas-配体中两个小孔蛋白结合位点的缺失削弱了其在细胞膜之间的分布,并减弱了Fas-配体诱导的细胞毒性。这些结果表明,Fas-配体和caveolin-1的相互作用代表了Fas-配体易位到木筏以及随后诱导的Fas-配体依赖性细胞死亡的分子基础。讨论了其他TNF家族成员和小窝蛋白1之间类似关联的可能性。

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