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蛋白质生物合成中的加工机制。

Processing mechanisms in the biosynthesis of proteins.

作者信息

Steiner D F, Quinn P S, Chan S J, Marsh J, Tager H S

出版信息

Ann N Y Acad Sci. 1980;343:1-16. doi: 10.1111/j.1749-6632.1980.tb47238.x.

Abstract

Limited proteolysis is a widely occurring mechanism in protein biosynthesis. Protein precursors can be classified according to their functions, localization within cell compartments, and enzymic cleavage mechanisms. The presecretory proteins represent an important class of very rapidly turning over precursors which play an early role in the sequestration of secretory products and whose cleavage appears to be intimately associated with structures formed at the ribosome-membrane junction during protein synthesis. A model is proposed which predicts that the prepeptide forms a beta-pleated sheet structure with other components of the membrane which results in the transfer of a loop of peptide across the microsomal membrane. Proinsulin is representative of the general class of proproteins that are processed post-translationally within their secretory cells either during the formation and maturation of secretory granules (peptides hormones and neurotransmitters, serum albumins) or during the assembly of macromolecular structures (virus capsules, membrane-associated enzyme complexes). The former group are cleaved by Golgi-associated proteases having tryptic and carboxypeptidase B-like specificity. Some precursors are secreted as such and processed extracellularly either in the circulation or at special sites (procollagens, zymogens, provenoms, vitellogenins).

摘要

有限蛋白水解是蛋白质生物合成中广泛存在的一种机制。蛋白质前体可根据其功能、在细胞区室中的定位以及酶切机制进行分类。分泌前体蛋白是一类重要的周转极快的前体,它们在分泌产物的隔离中起早期作用,其切割似乎与蛋白质合成过程中核糖体 - 膜交界处形成的结构密切相关。本文提出了一个模型,该模型预测前肽与膜的其他成分形成β - 折叠片层结构,导致一段肽环穿过微粒体膜。胰岛素原是一类前体蛋白的代表,这类前体蛋白在其分泌细胞内进行翻译后加工,加工过程要么发生在分泌颗粒形成和成熟期间(肽类激素和神经递质、血清白蛋白),要么发生在大分子结构组装期间(病毒衣壳、膜相关酶复合物)。前一组由具有胰蛋白酶和羧肽酶B样特异性的高尔基体相关蛋白酶切割。一些前体以这种形式分泌,并在循环中或特殊部位(前胶原、酶原、毒液、卵黄生成素)进行细胞外加工。

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