The activity of a human endoplasmic reticulum-associated degradation E3, gp78, requires its Cue domain,, RING finger, and an E2-binding site

Author:

Chen, B.

Mariano, J.

Tsai, Y. C.

Chan, A. H.

Cohen, M.

Weissman, A. M.
Author Address

NCI, Lab Prot Dynam & Signaling, Canc Res Ctr, Frederick, MD 21702 USA Weissman, AM, NCI, Lab Prot Dynam & Signaling, Canc Res Ctr, Bldg 560,Room 22-103, Frederick, MD 21702 USA

1. Year: 2006
2. Date: JAN 10
Journal: Proceedings of the National Academy of Sciences of the United States of America
1. Volume: 103
2. Issue: 2
3. Pages: 341-346
Type of Article: Article

Abstract:

Efficient targeting of proteins for degradation from the secretory pathway is essential to homeostasis. This occurs through endoplasmic reticulum (ER)-associated degradation (ERAD). In this study, we establish that a human ubiquitin ligase (E3), gp78, and a specific E2, Ube2g2, are both critically important for ERAD of multiple substrates. gp78 exhibits a complex domain structure that, in addition to the RING finger, includes a ubiquitin-binding Cue domain and a specific binding site for Ube2g2. Disruption of either of these domains abolishes gp78-mediated ubiquitylation and protein degradation, resulting in accumulation of substrates in their fully glycosylated forms in the ER. This suggests that gp78-mediated ubiquitylation is an early step in ERAD that precedes dislocation of substrates from the ER. The in vivo requirement for both an E2-bincling site distinct from the RING finger and a ubiquitin-binding domain intrinsic to an E3 suggests a previously unappreciated level of complexity in ubiquitin ligase function. These results also provide proof of principle that interrupting a specific E2-E3 interaction can selectively inhibit ERAD

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