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在危险环境中成长:胞质溶胶中新生多肽的多重靶向和折叠途径网络

Growing up in a dangerous environment: a network of multiple targeting and folding pathways for nascent polypeptides in the cytosol.

作者信息

Bukau B, Hesterkamp T, Luirink J

机构信息

Zentrum für Molekulare Biologie, Universität Heidelberg, Germany.

出版信息

Trends Cell Biol. 1996 Dec;6(12):480-6. doi: 10.1016/0962-8924(96)84946-4.

Abstract

The first events in the lives of proteins are the most hazardous. Starting at the ribosome, nascent polypeptides undergo complex folding processes endangered by aggregation reactions. Proteins with organellar destinations require correct targeting to the translocation machineries and prevention from premature folding. The high precision and speed of these processes is ensured by a cystosolic system consisting of molecular chaperones, folding catalysts and targeting factors. This review focuses on the interactions of this system with nascent polypeptides and discusses new concepts for protein folding in the cytosol. It is proposed that folding and targeting are promoted by a flexible network of multiple unassisted and assisted pathways.

摘要

蛋白质生命历程中的首个事件是最具风险的。从核糖体开始,新生多肽会经历受聚集反应威胁的复杂折叠过程。具有细胞器定位的蛋白质需要正确靶向转运机制并防止过早折叠。这些过程的高精度和速度由一个由分子伴侣、折叠催化剂和靶向因子组成的胞质系统来确保。本综述聚焦于该系统与新生多肽的相互作用,并讨论胞质中蛋白质折叠的新概念。有人提出,折叠和靶向是由多个无辅助和有辅助途径的灵活网络促进的。

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