On Jan 9, 2020, researchers at Pro. Xu’s lab published an article entitled “MCPIP1 inhibits Hepatitis B virus replication by destabilizing viral RNA and negatively regulates the virus-induced innate inflammatory responses” in Antiviral Research.
Monocyte chemotactic protein-induced protein 1 (MCPIP1) is an inflammatory regulator in immune response. Recently, MCPIP1 has also been identified as a host antiviral factor against certain virus infection including human immunodeficiency virus, dengue virus and hepatitis C virus. However, whether MCPIP1 could restrict the replication of hepatitis B virus (HBV), a DNA pararetrovirus belonging to Hepadnaviridae family, has not been investigated. In this study, we found that MCPIP1 expression was up-regulated in mouse livers upon acute HBV replication and in HBV-replicated hepatoma cells or HBV-stimulated macrophages. Enforced MCPIP1 expression by hydrodynamic DNA injection in vivo significantly inhibited HBV replication in the mouse livers. Then in vitro studies by overexpression or knockdown assays in cell-lines identified the direct antiviral effect of MCPIP1 on HBV replication. RNA immunoprecipitation and decay assay further suggested that MCPIP1 potently restricted HBV replication through directly binding viral RNA and degrading RNA via its RNase activity, but not deubiquitinase activity. Moreover, we further verified that MCPIP1 negatively regulated HBV-induced proinflammatory cytokines, such as IL-1β, TNF-α and IL-6 in macrophages. Taken together, our data expand MCPIP1's range of viral targets to DNA virus and also demonstrate the negative regulatory role of MCPIP1 in suppressing virus-induced inflammatory response, suggesting MCPIP1 as a potential therapeutic target for treating HBV related diseases via inducing a host defense against HBV and reducing inflammatory injury meanwhile.
Associated Prof. Min Li is the co-first author and co-corresponding authors. Dr. Candidate Jie Yang is co-first author. Prof. Wei Xu is the corresponding author. This work was supported by Chinese National Natural Science Foundation of China (31400769, 31870903, 31870868, and 31670930), Jiangsu Province Natural Science Foundation (BK20140371) and Jiangsu Postdoctor Science Foundation (1402176C), Priority Academic Program Development of Jiangsu Higher Education Institutions (PARD) and Jiangsu Provincial Innovative Research Team.