Author
Listed:
- Yong Wang
(Chinese Academy of Sciences
Chinese Academy of Sciences)
- Qi Zhan
(Chinese Academy of Sciences
Chinese Academy of Sciences
University of Chinese Academy of Sciences)
- Xinlu Wang
(Chinese Academy of Sciences)
- Peipei Li
(Chinese Academy of Sciences
Chinese Academy of Sciences
University of Chinese Academy of Sciences)
- Songqing Liu
(Chinese Academy of Sciences
Chinese Academy of Sciences)
- Guangxia Gao
(Chinese Academy of Sciences)
- Pu Gao
(Chinese Academy of Sciences
Chinese Academy of Sciences)
Abstract
The bacterial effector MavC catalyzes non-canonical ubiquitination of host E2 enzyme UBE2N without engaging any of the conventional ubiquitination machinery, thereby abolishing UBE2N’s function in forming K63-linked ubiquitin (Ub) chains and dampening NF-кB signaling. We now report the structures of MavC in complex with conjugated UBE2N~Ub and an inhibitor protein Lpg2149, as well as the structure of its ortholog, MvcA, bound to Lpg2149. Recognition of UBE2N and Ub depends on several unique features of MavC, which explains the inability of MvcA to catalyze ubiquitination. Unexpectedly, MavC and MvcA also possess deubiquitinase activity against MavC-mediated ubiquitination, highlighting MavC as a unique enzyme possessing deamidation, ubiquitination, and deubiquitination activities. Further, Lpg2149 directly binds and inhibits both MavC and MvcA by disrupting the interactions between enzymes and Ub. These results provide detailed insights into catalysis and regulation of MavC-type enzymes and the molecular mechanisms of this non-canonical ubiquitination machinery.
Suggested Citation
Yong Wang & Qi Zhan & Xinlu Wang & Peipei Li & Songqing Liu & Guangxia Gao & Pu Gao, 2020.
"Insights into catalysis and regulation of non-canonical ubiquitination and deubiquitination by bacterial deamidase effectors,"
Nature Communications, Nature, vol. 11(1), pages 1-13, December.
Handle:
RePEc:nat:natcom:v:11:y:2020:i:1:d:10.1038_s41467-020-16587-w
DOI: 10.1038/s41467-020-16587-w
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