OS-9 and GRP94 deliver mutant α1-antitrypsin to the Hrd1–SEL1L ubiquitin ligase complex for ERAD

John C. Christianson; Thomas A. Shaler; Ryan E. Tyler; Ron R. Kopito

doi:https://doi.org/10.1038/ncb1689

doi.org/10.1038/ncb1689

OS-9 and GRP94 deliver mutant α1-antitrypsin to the Hrd1–SEL1L ubiquitin ligase complex for ERAD

,

,

..., Ron R. Kopito

61

Nature Cell Biology21.30

Volume: 10, Issue: 3, Pages: 272 - 282

Published: Feb 10, 2008

Abstract

Terminally misfolded or unassembled proteins in the early secretory pathway are degraded by a ubiquitin- and proteasome-dependent process known as ER-associated degradation (ERAD). How substrates of this pathway are recognized within the ER and delivered to the cytoplasmic ubiquitin-conjugating machinery is unknown. We report here that OS-9 and XTP3-B/Erlectin are ER-resident glycoproteins that bind to ERAD substrates and, through the SEL1L...

Paper Fields

Paper Details

Title

OS-9 and GRP94 deliver mutant α1-antitrypsin to the Hrd1–SEL1L ubiquitin ligase complex for ERAD

DOI

doi.org/10.1038/ncb1689

Published Date

Feb 10, 2008

Journal

Nature Cell Biology

Volume

10

Issue

3

Pages

272 - 282

Citation AnalysisPro

You’ll need to upgrade your plan to Pro

Looking to understand the true influence of a researcher’s work across journals & affiliations?

Scinapse’s Top 10 Citation Journals & Affiliations graph reveals the quality and authenticity of citations received by a paper.
Discover whether citations have been inflated due to self-citations, or if citations include institutional bias.

Learn more

Notes

History