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内质网膜复合体的冷冻电镜结构

Cryo-EM structures of the endoplasmic reticulum membrane complex.

作者信息

Bai Lin, Li Huilin

机构信息

Department of Biochemistry and Biophysics, School of Basic Medical Sciences, Peking University, Beijing, China.

Department of Structural Biology, Van Andel Institute, Grand Rapids, MI, USA.

出版信息

FEBS J. 2022 Jan;289(1):102-112. doi: 10.1111/febs.15786. Epub 2021 Mar 6.

Abstract

The transmembrane α-helices of membrane proteins are in general highly hydrophobic, and they enter the lipid bilayer through a lateral gate in the Sec61 translocon. However, some transmembrane α-helices are less hydrophobic and form membrane channels or substrate-binding pockets. Insertion of these amphipathic transmembrane α-helices into the membrane requires the specific membrane-embedded insertase called the endoplasmic reticulum membrane complex (EMC), which is a multi-subunit chaperone distinct from the GET insertase complex. Four recent cryo-electron microscopy studies on the eukaryotic EMC have revealed their remarkable architectural conservation from yeast to humans; a general consensus on the substrate transmembrane helix-binding pocket; and the evolutionary link to the prokaryotic insertases of the tail-anchored membrane proteins. These structures provide a solid framework for future mechanistic investigation.

摘要

膜蛋白的跨膜α螺旋通常具有高度疏水性,它们通过Sec61转运体的侧向门进入脂质双层。然而,一些跨膜α螺旋疏水性较低,会形成膜通道或底物结合口袋。将这些两亲性跨膜α螺旋插入膜中需要一种特定的膜嵌入插入酶,即内质网膜复合体(EMC),它是一种与GET插入酶复合体不同的多亚基伴侣蛋白。最近四项关于真核生物EMC的冷冻电子显微镜研究揭示了其从酵母到人类显著的结构保守性;对底物跨膜螺旋结合口袋的普遍共识;以及与尾锚定膜蛋白的原核插入酶的进化联系。这些结构为未来的机制研究提供了坚实的框架。

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