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The mitochondrial ubiquitin ligase MARCH5 resolves MAVS aggregates during antiviral signalling.

Authors
Yoo, YS | Park, YY  | Kim, JH | Cho, H  | Kim, SH | Lee, HS | Kim, TH | Kim, YS  | Lee, Y  | Kim, CJ | Jung, JU | Lee, JS
Citation
Nature communications, 6. : 7910-7910, 2015
Journal Title
Nature communications
ISSN
2041-1723
Abstract
Mitochondria serve as platforms for innate immunity. The mitochondrial antiviral signalling (MAVS) protein forms aggregates that elicit robust type-I interferon induction on viral infection, but persistent MAVS signalling leads to host immunopathology; it remains unknown how these signalling aggregates are resolved. Here we identify the mitochondria-resident E3 ligase, MARCH5, as a negative regulator of MAVS aggregates. March5(+/-) mice and MARCH5-deficient immune cells exhibit low viral replication and elevated type-I interferon responses to RNA viruses. MARCH5 binds MAVS only during viral stimulation when MAVS forms aggregates, and these interactions require the RING domain of MARCH5 and the CARD domain of MAVS. MARCH5, but not its RING mutant (MARCH5(H43W)), reduces the level of MAVS aggregates. MARCH5 transfers ubiquitin to Lys7 and Lys500 of MAVS and promotes its proteasome-mediated degradation. Our results indicate that MARCH5 modulates MAVS-mediated antiviral signalling, preventing excessive immune reactions.
MeSH

DOI
10.1038/ncomms8910
PMID
26246171
Appears in Collections:
Journal Papers > School of Medicine / Graduate School of Medicine > Biochemistry & Molecular Biology
Journal Papers > Research Organization > Institute for Medical Sciences
Ajou Authors
김, 유선  |  박, 용예  |  이, 영수  |  조, 혜성
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