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蛋白质向人内质网的转运。

Protein transport into the human endoplasmic reticulum.

机构信息

Medical Biochemistry and Molecular Biology, Saarland University, 66421 Homburg, Germany.

Department of Molecular Structural Biology, Max Planck Institute of Biochemistry, 82152 Martinsried, Germany.

出版信息

J Mol Biol. 2015 Mar 27;427(6 Pt A):1159-75. doi: 10.1016/j.jmb.2014.06.011. Epub 2014 Jun 23.

Abstract

Protein transport into the endoplasmic reticulum (ER) is essential for all eukaryotic cells and evolutionary related to protein transport into and across the cytoplasmic membrane of eubacteria and archaea. It is based on amino-terminal signal peptides in the precursor polypeptides plus various transport components in cytosol plus ER and can occur either cotranslationally or posttranslationally. The two mechanisms merge at the heterotrimeric Sec61 complex in the ER membrane, which forms an aqueous polypeptide-conducting channel. Since the mammalian ER is also the main intracellular calcium storage organelle, the Sec61 complex is tightly regulated in its dynamics between the open and closed conformations by various ligands, such as precursor polypeptides at the cytosolic face and the Hsp70-type molecular chaperone BiP at the ER lumenal face (Hsp, heat shock protein). Furthermore, BiP binding to the incoming precursor polypeptide contributes to unidirectionality and efficiency of transport. Recent insights into the structural dynamics of the Sec61 complex and related complexes in eubacteria and archaea have various mechanistic and functional implications.

摘要

蛋白质向内质网(ER)的转运对于所有真核细胞都是必不可少的,并且与原核生物和古菌细胞质膜中的蛋白质转运在进化上是相关的。它基于前体多肽中的氨基末端信号肽,加上细胞质和 ER 中的各种转运成分,并且可以共翻译或翻译后发生。这两种机制在 ER 膜中的三聚体 Sec61 复合物中融合,该复合物形成一个水相多肽传导通道。由于哺乳动物 ER 也是主要的细胞内钙储存细胞器,因此各种配体(如细胞质侧的前体多肽和 ER 腔内腔面的 Hsp70 型分子伴侣 BiP(Hsp,热休克蛋白))紧密调节 Sec61 复合物在开放和关闭构象之间的动力学。此外,BiP 与进入的前体多肽的结合有助于运输的单向性和效率。最近对原核生物和古菌中的 Sec61 复合物和相关复合物的结构动力学的深入了解具有各种机制和功能意义。

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