A non-canonical role of the p97 complex in RIG-I antiviral signaling.

نویسندگان

  • Qian Hao
  • Shi Jiao
  • Zhubing Shi
  • Chuanchuan Li
  • Xia Meng
  • Zhen Zhang
  • Yanyan Wang
  • Xiaomin Song
  • Wenjia Wang
  • Rongguang Zhang
  • Yun Zhao
  • Catherine C L Wong
  • Zhaocai Zhou
چکیده

RIG-I is a well-studied sensor of viral RNA that plays a key role in innate immunity. p97 regulates a variety of cellular events such as protein quality control, membrane reassembly, DNA repair, and the cell cycle. Here, we report a new role for p97 with Npl4-Ufd1 as its cofactor in reducing antiviral innate immune responses by facilitating proteasomal degradation of RIG-I. The p97 complex is able to directly bind both non-ubiquitinated RIG-I and the E3 ligase RNF125, promoting K48-linked ubiquitination of RIG-I at residue K181. Viral infection significantly strengthens the interaction between RIG-I and the p97 complex by a conformational change of RIG-I that exposes the CARDs and through K63-linked ubiquitination of these CARDs. Disruption of the p97 complex enhances RIG-I antiviral signaling. Consistently, administration of compounds targeting p97 ATPase activity was shown to inhibit viral replication and protect mice from vesicular stomatitis virus (VSV) infection. Overall, our study uncovered a previously unrecognized role for the p97 complex in protein ubiquitination and revealed the p97 complex as a potential drug target in antiviral therapy.

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عنوان ژورنال:
  • The EMBO journal

دوره 34 23  شماره 

صفحات  -

تاریخ انتشار 2015