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Fingerloop activates cargo delivery and unloading during cotranslational protein targeting

机译:Fingerloop在共翻译蛋白靶向过程中激活了货物的运输和卸载

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During cotranslational protein targeting by the signal recognition particle (SRP), information about signal sequence binding in the SRP's M domain must be effectively communicated to its GTPase domain to turn on its interaction with the SRP receptor (SR) and thus deliver the cargo proteins to the membrane. A universally conserved “fingerloop” lines the signal sequence–binding groove of SRP; the precise role of this fingerloop in protein targeting has remained elusive. In this study, we show that the fingerloop plays important roles in SRP function by helping to induce the SRP into a more active conformation that facilitates multiple steps in the pathway, including efficient recruitment of SR, GTPase activation in the SRP?SR complex, and most significantly, the unloading of cargo onto the target membrane. On the basis of these results and recent structural work, we propose that the fingerloop is the first structural element to detect signal sequence binding; this information is relayed to the linker connecting the SRP's M and G domains and thus activates the SRP and SR for carrying out downstream steps in the pathway.
机译:在信号识别颗粒(SRP)进行共翻译蛋白靶向的过程中,必须将有关SRP M结构域中信号序列结合的信息有效地传递至其GTPase结构域,以开启其与SRP受体(SR)的相互作用,从而将货物蛋白传递给膜。 SRP的信号序列绑定凹槽处普遍保留了“指环”。这种指环在蛋白质靶向中的确切作用仍然难以捉摸。在这项研究中,我们证明了指环在SRP功能中起着重要作用,它可以帮助将SRP诱导为更活跃的构象,从而促进该途径的多个步骤,包括有效募集SR,SRP?SR复合物中的GTPase活化以及最重要的是,将货物卸载到目标膜上。根据这些结果和最近的结构研究,我们建议指环是检测信号序列结合的第一个结构元件。该信息被中继到连接SRP的M和G域的链接器,从而激活SRP和SR以执行路径中的下游步骤。

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