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在内质网和高尔基体复合体之间运送膜蛋白。

Getting membrane proteins on and off the shuttle bus between the endoplasmic reticulum and the Golgi complex.

作者信息

Borgese Nica

机构信息

CNR Institute of Neuroscience, Milan 20129, Italy

出版信息

J Cell Sci. 2016 Apr 15;129(8):1537-45. doi: 10.1242/jcs.183335. Epub 2016 Mar 30.

DOI:10.1242/jcs.183335
PMID:27029344
Abstract

Secretory proteins exit the endoplasmic reticulum (ER) in coat protein complex II (COPII)-coated vesicles and then progress through the Golgi complex before delivery to their final destination. Soluble cargo can be recruited to ER exit sites by signal-mediated processes (cargo capture) or by bulk flow. For membrane proteins, a third mechanism, based on the interaction of their transmembrane domain (TMD) with lipid microdomains, must also be considered. In this Commentary, I review evidence in favor of the idea that partitioning of TMDs into bilayer domains that are endowed with distinct physico-chemical properties plays a pivotal role in the transport of membrane proteins within the early secretory pathway. The combination of such self-organizational phenomena with canonical intermolecular interactions is most likely to control the release of membrane proteins from the ER into the secretory pathway.

摘要

分泌蛋白通过包被蛋白复合物II(COPII)包被的囊泡离开内质网(ER),然后在被运送到最终目的地之前经过高尔基体复合体。可溶性货物可以通过信号介导的过程(货物捕获)或通过整体流动被募集到内质网出口位点。对于膜蛋白,还必须考虑基于其跨膜结构域(TMD)与脂质微区相互作用的第三种机制。在这篇评论中,我回顾了支持以下观点的证据:将TMD分配到具有不同物理化学性质的双层结构域中,在早期分泌途径中膜蛋白的运输中起关键作用。这种自组织现象与典型分子间相互作用的结合最有可能控制膜蛋白从内质网释放到分泌途径中。

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