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触发因子是一种真正的分泌途径伴侣蛋白,它与 SecB 和易位酶相互作用。

Trigger factor is a bona fide secretory pathway chaperone that interacts with SecB and the translocase.

机构信息

Department of Microbiology and Immunology, Rega Institute for Medical Research, Laboratory of Molecular Bacteriology, KU Leuven, Leuven, Belgium.

出版信息

EMBO Rep. 2020 Jun 4;21(6):e49054. doi: 10.15252/embr.201949054. Epub 2020 Apr 19.

Abstract

Bacterial secretory preproteins are translocated across the inner membrane post-translationally by the SecYEG-SecA translocase. Mature domain features and signal peptides maintain preproteins in kinetically trapped, largely soluble, folding intermediates. Some aggregation-prone preproteins require chaperones, like trigger factor (TF) and SecB, for solubility and/or targeting. TF antagonizes the contribution of SecB to secretion by an unknown molecular mechanism. We reconstituted this interaction in vitro and studied targeting and secretion of the model preprotein pro-OmpA. TF and SecB display distinct, unsuspected roles in secretion. Tightly associating TF:pro-OmpA targets the translocase at SecA, but TF prevents pro-OmpA secretion. In solution, SecB binds TF:pro-OmpA with high affinity. At the membrane, when bound to the SecA C-tail, SecB increases TF and TF:pro-OmpA affinities for the translocase and allows pro-OmpA to resume translocation. Our data reveal that TF, a main cytoplasmic folding pathway chaperone, is also a bona fide post-translational secretory chaperone that directly interacts with both SecB and the translocase to mediate regulated protein secretion. Thus, TF links the cytoplasmic folding and secretion chaperone networks.

摘要

细菌分泌前体蛋白在翻译后通过 SecYEG-SecA 转运体穿过内膜转运。成熟结构域特征和信号肽使前体蛋白保持在动力学捕获的、大部分可溶性的折叠中间体中。一些容易聚集的前体蛋白需要伴侣蛋白,如触发因子(TF)和 SecB,以保持可溶性和/或靶向性。TF 通过未知的分子机制拮抗 SecB 对分泌的贡献。我们在体外重建了这种相互作用,并研究了模型前体蛋白 pro-OmpA 的靶向和分泌。TF 和 SecB 在分泌中表现出不同的、意想不到的作用。紧密结合的 TF:pro-OmpA 将转运体靶向 SecA,但 TF 阻止 pro-OmpA 分泌。在溶液中,SecB 与 TF:pro-OmpA 具有高亲和力结合。在膜上,当与 SecA C 尾结合时,SecB 增加了 TF 和 TF:pro-OmpA 与转运体的亲和力,并允许 pro-OmpA 重新开始易位。我们的数据表明,TF,一种主要的细胞质折叠途径伴侣蛋白,也是一种真正的翻译后分泌伴侣蛋白,它直接与 SecB 和转运体相互作用,介导受调控的蛋白质分泌。因此,TF 连接了细胞质折叠和分泌伴侣蛋白网络。

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