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Toc75 的 POTRA 结构域具有伴侣蛋白样功能,有助于其进入叶绿体。

The POTRA domains of Toc75 exhibit chaperone-like function to facilitate import into chloroplasts.

机构信息

Markey Center for Structural Biology, Department of Biological Sciences, Purdue University, West Lafayette, IN 47907.

Purdue Institute of Inflammation, Immunology and Infectious Disease, Purdue University, West Lafayette, IN 47907.

出版信息

Proc Natl Acad Sci U S A. 2017 Jun 13;114(24):E4868-E4876. doi: 10.1073/pnas.1621179114. Epub 2017 May 30.

Abstract

Protein trafficking across membranes is an essential function in cells; however, the exact mechanism for how this occurs is not well understood. In the endosymbionts, mitochondria and chloroplasts, the vast majority of proteins are synthesized in the cytoplasm as preproteins and then imported into the organelles via specialized machineries. In chloroplasts, protein import is accomplished by the TOC (translocon on the outer chloroplast membrane) and TIC (translocon on the inner chloroplast membrane) machineries in the outer and inner envelope membranes, respectively. TOC mediates initial recognition of preproteins at the outer membrane and includes a core membrane channel, Toc75, and two receptor proteins, Toc33/34 and Toc159, each containing GTPase domains that control preprotein binding and translocation. Toc75 is predicted to have a β-barrel fold consisting of an N-terminal intermembrane space (IMS) domain and a C-terminal 16-stranded β-barrel domain. Here we report the crystal structure of the N-terminal IMS domain of Toc75 from , revealing three tandem polypeptide transport-associated (POTRA) domains, with POTRA2 containing an additional elongated helix not observed previously in other POTRA domains. Functional studies show an interaction with the preprotein, preSSU, which is mediated through POTRA2-3. POTRA2-3 also was found to have chaperone-like activity in an insulin aggregation assay, which we propose facilitates preprotein import. Our data suggest a model in which the POTRA domains serve as a binding site for the preprotein as it emerges from the Toc75 channel and provide a chaperone-like activity to prevent misfolding or aggregation as the preprotein traverses the intermembrane space.

摘要

蛋白质跨膜运输是细胞中一种重要的功能;然而,其具体机制尚不清楚。在内共生体中,线粒体和叶绿体中的绝大多数蛋白质都是作为前体蛋白在细胞质中合成的,然后通过专门的机制导入细胞器。在叶绿体中,蛋白质的导入是通过外膜上的 TOC(跨膜转运器)和内膜上的 TIC(跨膜转运器)机制来完成的。TOC 介导前体蛋白在外膜上的初步识别,包括一个核心膜通道 Toc75 和两个受体蛋白 Toc33/34 和 Toc159,它们都含有 GTPase 结构域,控制前体蛋白的结合和转运。Toc75 被预测具有由 N 端膜间隙(IMS)结构域和 C 端 16 股 β-桶结构域组成的 β-桶折叠。在这里,我们报告了来自 的 Toc75 的 N 端 IMS 结构域的晶体结构,揭示了三个串联的多肽转运相关(POTRA)结构域,其中 POTRA2 含有一个以前在其他 POTRA 结构域中未观察到的额外延长的螺旋。功能研究表明,与前体蛋白 preSSU 相互作用,该相互作用是通过 POTRA2-3 介导的。POTRA2-3 在胰岛素聚集测定中也具有伴侣样活性,我们认为这有助于前体蛋白的导入。我们的数据表明,POTRA 结构域作为前体蛋白从 Toc75 通道中出现时的结合位点,提供伴侣样活性以防止前体蛋白在穿过膜间隙时错误折叠或聚集。

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