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共翻译转运至内质网的起源与进化。

Origins and evolution of cotranslational transport to the ER.

作者信息

Schwartz Thomas U

机构信息

Department of Biology, Massachusetts Institute of Technology, 77 Massachusetts Avenue, Cambridge, Massachusetts 02139, USA.

出版信息

Adv Exp Med Biol. 2007;607:52-60. doi: 10.1007/978-0-387-74021-8_4.

Abstract

All living organisms possess the ability to translocate proteins across biological membranes. This is a fundamental necessity since proteins function in different locations yet are synthesized in one compartment only, the cytosol. Even though different transport systems exist, the pathway that is dominantly used to translocate secretory and membrane proteins is known as the cotranslational transport pathway. It evolved only once and is in its core conserved throughout all kingdoms of life. The process is characterized by a well understood sequence of events: first, an N-terminal signal sequence of a nascent polypeptide is recognized on the ribosome by the signal recognition particle (SRP), then the SRP-ribosome complex is targeted to the membrane via the SRP receptor. Next, the nascent chain is transferred from SRP to the protein conducting channel, through which it is cotranslationally threaded. All the essential components of the system have been identified. Recent structural and biochemical studies have unveiled some of the intricate regulatory circuitry of the process. These studies also shed light on the accessory components unique to eukaryotes, pointing to early events in eukaryotic evolution.

摘要

所有生物都具备将蛋白质转运穿过生物膜的能力。这是一项基本需求,因为蛋白质在不同位置发挥功能,但仅在一个区室(即胞质溶胶)中合成。尽管存在不同的转运系统,但用于转运分泌蛋白和膜蛋白的主要途径被称为共翻译转运途径。它仅进化过一次,并且在其核心部分在所有生命王国中都是保守的。该过程的特点是一系列事件得到了很好的理解:首先,新生多肽的N端信号序列在核糖体上被信号识别颗粒(SRP)识别,然后SRP-核糖体复合物通过SRP受体靶向到膜上。接下来,新生链从SRP转移到蛋白质传导通道,通过该通道它被共翻译穿膜。该系统的所有基本组件都已被鉴定出来。最近的结构和生化研究揭示了该过程一些复杂的调控机制。这些研究还揭示了真核生物特有的辅助组件,指出了真核生物进化中的早期事件。

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