Cell Reports (Mar 2016)

CARMA3 Is a Host Factor Regulating the Balance of Inflammatory and Antiviral Responses against Viral Infection

  • Changying Jiang,
  • Zhicheng Zhou,
  • Yanping Quan,
  • Shilei Zhang,
  • Tingting Wang,
  • Xueqiang Zhao,
  • Clayton Morrison,
  • Mark T. Heise,
  • Wenqian He,
  • Matthew S. Miller,
  • Xin Lin

DOI
https://doi.org/10.1016/j.celrep.2016.02.031
Journal volume & issue
Vol. 14, no. 10
pp. 2389 – 2401

Abstract

Read online

Host response to RNA virus infection is sensed by RNA sensors such as RIG-I, which induces MAVS-mediated NF-κB and IRF3 activation to promote inflammatory and antiviral responses, respectively. Here, we have found that CARMA3, a scaffold protein previously shown to mediate NF-κB activation induced by GPCR and EGFR, positively regulates MAVS-induced NF-κB activation. However, our data suggest that CARMA3 sequesters MAVS from forming high-molecular-weight aggregates, thereby suppressing TBK1/IRF3 activation. Interestingly, following NF-κB activation upon virus infection, CARMA3 is targeted for proteasome-dependent degradation, which releases MAVS to activate IRF3. When challenged with vesicular stomatitis virus or influenza A virus, CARMA3-deficient mice showed reduced disease symptoms compared to those of wild-type mice as a result of less inflammation and a stronger ability to clear infected virus. Altogether, our results reveal the role of CARMA3 in regulating the balance of host antiviral and pro-inflammatory responses against RNA virus infection.

Keywords