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The conserved bardet-biedl syndrome proteins assemble a coat that traffics membrane proteins to Cilia

机译:保守的Bardet-Biedle综合征蛋白组装了一层将膜蛋白运输到纤毛的外套

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摘要

The BBSome is a complex of Bardet-Biedl Syndrome (BBS) proteins that shares common structural elements with COPI, COPII, and clathrin coats. Here, we show that the BBSome constitutes a coat complex that sorts membrane proteins to primary cilia. The BBSome is the major effector of the Arf-like GTPase Arl6/BBS3, and the BBSome and GTP-bound Arl6 colocalize at ciliary punctae in an interdependent manner. Strikingly, Arl6~(GTP)-mediated recruitment of the BBSome to synthetic liposomes produces distinct patches of polymerized coat apposed onto the lipid bilayer. Finally, the ciliary targeting signal of somatostatin receptor 3 needs to be directly recognized by the BBSome in order to mediate targeting of membrane proteins to cilia. Thus, we propose that trafficking of BBSome cargoes to cilia entails the coupling of BBSome coat polymerization to the recognition of sorting signals by the BBSome.
机译:BBSome是Bardet-Biedl综合征(BBS)蛋白的复合物,与COPI,COPII和网格蛋白外壳具有共同的结构元素。在这里,我们表明BBSome构成了一个外壳复合物,该复合物将膜蛋白分选到初级纤毛。 BBSome是类似Arf的GTPase Arl6 / BBS3的主要效应子,BBSome和GTP结合的Arl6以相互依赖的方式共定位于睫状突点。引人注目的是,Arl6-(GTP)介导的BBSome募集到合成脂质体上,产生了明显的贴在脂质双层上的聚合涂层斑块。最后,生长激素抑制素受体3的纤毛靶向信号需要被BBSome直接识别,以介导膜蛋白靶向纤毛。因此,我们建议将BBSome货物运至纤毛必须将BBSome涂层聚合与BBSome识别分拣信号相结合。

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