| Literature DB >> 35982226 |
Xiao Liang1, Jun Xiao1,2, Xuzichao Li1, Yujie Liu2, Yao Lu2, Yanan Wen1, Zexing Li3, Xing Che4, Yongjian Ma1, Xingyan Zhang1, Yi Zhang1, Deng Jian5, Peihui Wang5, Chenghao Xuan1, Guimei Yu6, Long Li7,8, Heng Zhang9.
Abstract
The E3 ligase TRIM7 has emerged as a critical player in viral infection and pathogenesis. However, the mechanism governing the TRIM7-substrate association remains to be defined. Here we report the crystal structures of TRIM7 in complex with 2C peptides of human enterovirus. Structure-guided studies reveal the C-terminal glutamine residue of 2C as the primary determinant for TRIM7 binding. Leveraged by this finding, we identify norovirus and SARS-CoV-2 proteins, and physiological proteins, as new TRIM7 substrates. Crystal structures of TRIM7 in complex with multiple peptides derived from SARS-CoV-2 proteins display the same glutamine-end recognition mode. Furthermore, TRIM7 could trigger the ubiquitination and degradation of these substrates, possibly representing a new Gln/C-degron pathway. Together, these findings unveil a common recognition mode by TRIM7, providing the foundation for further mechanistic characterization of antiviral and cellular functions of TRIM7.Entities:
Year: 2022 PMID: 35982226 DOI: 10.1038/s41589-022-01128-x
Source DB: PubMed Journal: Nat Chem Biol ISSN: 1552-4450 Impact factor: 16.174