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整合膜蛋白的可溶性前体:感染噬菌体M13的大肠杆菌中前衣壳蛋白的合成。

Soluble precursor of an integral membrane protein: synthesis of procoat protein in Escherichia coli infected with bacteriophage M13.

作者信息

Ito K, Mandel G, Wickner W

出版信息

Proc Natl Acad Sci U S A. 1979 Mar;76(3):1199-203. doi: 10.1073/pnas.76.3.1199.

Abstract

Prior to virus assembly, the major coat protein of coliphage M13 is an integral protein of the host cytoplasmic membrane. Coat protein synthesized in vitro is initially made with an NH2-terminal "leader peptide" of 23 amino acids and is termed "procoat." We now report that procoat is a biosynthetic precursor of coat protein in vivo. Conversion of procoat to coat occurs within 30 sec in cells infected with wild-type virus. This proteolytic processing is delayed in cells infected by M13 mutants (in genes 1, 5, or 7) that are defective in virus assembly. Pulse--chase experiments in combination with subcellular fractionation show that procoat is synthesized in a soluble form in the cytoplasm and is then incorporated into the cytoplasmic membrane, where it is converted to coat protein. This finding is supported by the observation that procoat is synthesized exclusively by polysomes that are not membrane bound. These results are interpreted in terms of the "membrane-triggered folding" hypothesis of membrane protein assembly.

摘要

在病毒组装之前,大肠杆菌噬菌体M13的主要衣壳蛋白是宿主细胞质膜的整合蛋白。体外合成的衣壳蛋白最初带有一个由23个氨基酸组成的NH2末端“前导肽”,被称为“前衣壳蛋白”。我们现在报告,前衣壳蛋白在体内是衣壳蛋白的生物合成前体。在感染野生型病毒的细胞中,前衣壳蛋白转化为衣壳蛋白的过程在30秒内发生。这种蛋白水解加工在感染了M13突变体(基因1、5或7)的细胞中延迟,这些突变体在病毒组装方面存在缺陷。脉冲追踪实验与亚细胞分级分离相结合表明,前衣壳蛋白在细胞质中以可溶形式合成,然后整合到细胞质膜中,在那里它被转化为衣壳蛋白。这一发现得到了以下观察结果的支持:前衣壳蛋白仅由不与膜结合的多核糖体合成。这些结果根据膜蛋白组装的“膜触发折叠”假说来解释。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3ec4/383217/c77f54f70ca1/pnas00003-0198-a.jpg

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