Literature DB >> 33236988

Structural and mechanistic basis of the EMC-dependent biogenesis of distinct transmembrane clients.

Lakshmi E Miller-Vedam1,2,3,4, Bastian Bräuning5, Katerina D Popova3,4,6, Nicole T Schirle Oakdale4, Jessica L Bonnar3,4, Jesuraj R Prabu5, Elizabeth A Boydston4, Natalia Sevillano7, Matthew J Shurtleff4, Robert M Stroud2, Charles S Craik7, Brenda A Schulman5, Adam Frost2, Jonathan S Weissman3,4,8.   

Abstract

Membrane protein biogenesis in the endoplasmic reticulum (ER) is complex and failure-prone. The ER membrane protein complex (EMC), comprising eight conserved subunits, has emerged as a central player in this process. Yet, we have limited understanding of how EMC enables insertion and integrity of diverse clients, from tail-anchored to polytopic transmembrane proteins. Here, yeast and human EMC cryo-EM structures reveal conserved intricate assemblies and human-specific features associated with pathologies. Structure-based functional studies distinguish between two separable EMC activities, as an insertase regulating tail-anchored protein levels and a broader role in polytopic membrane protein biogenesis. These depend on mechanistically coupled yet spatially distinct regions including two lipid-accessible membrane cavities which confer client-specific regulation, and a non-insertase EMC function mediated by the EMC lumenal domain. Our studies illuminate the structural and mechanistic basis of EMC's multifunctionality and point to its role in differentially regulating the biogenesis of distinct client protein classes.
© 2020, Miller-Vedam et al.

Entities:  

Keywords:  EMC; S. cerevisiae; cell biology; chaperone holdase; electron microscopy; endoplasmic reticulum; human; insertase; membrane protein biogenesis; molecular biophysics; structural biology

Mesh:

Substances:

Year:  2020        PMID: 33236988      PMCID: PMC7785296          DOI: 10.7554/eLife.62611

Source DB:  PubMed          Journal:  Elife        ISSN: 2050-084X            Impact factor:   8.140


  127 in total

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