Zinc-Finger Antiviral Protein Inhibits XMRV Infection

Abstract: Background The zinc-finger antiviral protein (ZAP) is a host factor that specifically inhibits the replication of certain viruses, including Moloney murine leukemia virus (MoMLV), HIV-1, and certain alphaviruses and filoviruses. ZAP binds to specific viral mRNAs and recruits cellular mRNA degradation machinery to degrade the target RNA. The common features of ZAP-responsive RNA sequences remain elusive and thus whether a virus is susceptible to ZAP can only be determined experimentally. Xenotropic… Show more

“…5 and 6). Additionally, we also evaluated whether ZAP inhibited CVB3 replication by activating RIG-I signaling and found knockdown of RIG-I in HeLa cells did not influence the antiviral effect of ZAP (data not shown), which is consistent with report of ZAP effect against XMRV (Wang, Tu et al, 2012). We also failed to detect any increase of IFN expression after overexpression of ZAP in vivo (Fig.…”

“…ZAP has been reported to suppress the replication of positive-stranded RNA viruses (Alphavirus and Flavivirus of Togaviridae), negativestranded RNA viruses (Filoviridae such as EBOV and MARV) and retroviruses (Retroviridae such as HIV, HBV and MMLV) in human cell lines. However, ZAP did not exhibit a broad-spectrum antiviral state in some viruses, including VSV, poliovirus and yellow fever virus, replicated to normal levels in ZAP-expressing cells (Muller, Moller et al, 2007;Zhu, Chen et al, 2011;Wang, Tu et al, 2012;Xuan, Liu et al, 2012;Mao, Nie et al, 2013;Chen, Dai et al, 2015). CVB3 and poliovirus are members of the positive-stranded RNA virus family picornaviridae, effect of ZAP on CVB3 replication has never been reported.…”

“…Previous studies have demonstrated that ZAP prevents the accumulation of viral RNA by targeting specific sequences mostly found in 3 0 or 5 0 untranslated region (UTR) of viral RNA (Zhu, Chen et al, 2011;Wang, Tu et al, 2012). To identify the target sequences of ZAP in CVB3 genome, the 3 0 UTR and 5 0 UTR of CVB3 were cloned into the pGL3-luciferase reporter plasmid respectively (Fig.…”

“…Human ZAP has a long and a short isoform (hZAP-L and -S) resulting from different mRNA splicing and both of them are reported to restrict replication of RNA viruses such as alphaviruses, floviruses and retroviruses including human immunodeficiency virus (HIV), hepatitis B virus (HBV), xenotropic murine leukemia virus-related virus (XMRV). However, ZAP does not exhibit antiviral effect commonly to all viruses, some viruses such as vesicular stomatitis virus (VSV), poliovirus and yellow fever virus, replicate normally in ZAP-overexpressed cells (Muller, Moller et al, 2007;Zhu, Chen et al, 2011;Wang, Tu et al, 2012;Xuan, Liu et al, 2012;Mao, Nie et al, 2013;Chen, Dai et al, 2015). ZAP is demonstrated to exert its antiviral effect by binding to viral RNA through its CCCH zinc finger motif and recruiting host RNA exosome or cellular decapping complex to degrade viral RNA in the cytoplasm (Guo, Carroll et al, 2004;Lee, Komano et al, 2013).…”

“…ZAP is demonstrated to exert its antiviral effect by binding to viral RNA through its CCCH zinc finger motif and recruiting host RNA exosome or cellular decapping complex to degrade viral RNA in the cytoplasm (Guo, Carroll et al, 2004;Lee, Komano et al, 2013). The ZAPresponsive elements (ZREs) vary among viral RNAs (Guo, Carroll et al, 2004;Zhu, Chen et al, 2011;Wang, Tu et al, 2012). Since there is no report of the effect of ZAP on enteroviruses infection and almost no biological function of ZAP has been confirmed in animal models of viral infection, it is of great interest to explore the possible antiviral function of ZAP on CVB3 and role of ZAP in the development of CVB3-induced acute viral myocarditis (VMC).…”

Zinc finger antiviral protein inhibits coxsackievirus B3 virus replication and protects against viral myocarditis

“…5 and 6). Additionally, we also evaluated whether ZAP inhibited CVB3 replication by activating RIG-I signaling and found knockdown of RIG-I in HeLa cells did not influence the antiviral effect of ZAP (data not shown), which is consistent with report of ZAP effect against XMRV (Wang, Tu et al, 2012). We also failed to detect any increase of IFN expression after overexpression of ZAP in vivo (Fig.…”

“…ZAP has been reported to suppress the replication of positive-stranded RNA viruses (Alphavirus and Flavivirus of Togaviridae), negativestranded RNA viruses (Filoviridae such as EBOV and MARV) and retroviruses (Retroviridae such as HIV, HBV and MMLV) in human cell lines. However, ZAP did not exhibit a broad-spectrum antiviral state in some viruses, including VSV, poliovirus and yellow fever virus, replicated to normal levels in ZAP-expressing cells (Muller, Moller et al, 2007;Zhu, Chen et al, 2011;Wang, Tu et al, 2012;Xuan, Liu et al, 2012;Mao, Nie et al, 2013;Chen, Dai et al, 2015). CVB3 and poliovirus are members of the positive-stranded RNA virus family picornaviridae, effect of ZAP on CVB3 replication has never been reported.…”

“…Previous studies have demonstrated that ZAP prevents the accumulation of viral RNA by targeting specific sequences mostly found in 3 0 or 5 0 untranslated region (UTR) of viral RNA (Zhu, Chen et al, 2011;Wang, Tu et al, 2012). To identify the target sequences of ZAP in CVB3 genome, the 3 0 UTR and 5 0 UTR of CVB3 were cloned into the pGL3-luciferase reporter plasmid respectively (Fig.…”

“…Human ZAP has a long and a short isoform (hZAP-L and -S) resulting from different mRNA splicing and both of them are reported to restrict replication of RNA viruses such as alphaviruses, floviruses and retroviruses including human immunodeficiency virus (HIV), hepatitis B virus (HBV), xenotropic murine leukemia virus-related virus (XMRV). However, ZAP does not exhibit antiviral effect commonly to all viruses, some viruses such as vesicular stomatitis virus (VSV), poliovirus and yellow fever virus, replicate normally in ZAP-overexpressed cells (Muller, Moller et al, 2007;Zhu, Chen et al, 2011;Wang, Tu et al, 2012;Xuan, Liu et al, 2012;Mao, Nie et al, 2013;Chen, Dai et al, 2015). ZAP is demonstrated to exert its antiviral effect by binding to viral RNA through its CCCH zinc finger motif and recruiting host RNA exosome or cellular decapping complex to degrade viral RNA in the cytoplasm (Guo, Carroll et al, 2004;Lee, Komano et al, 2013).…”

“…ZAP is demonstrated to exert its antiviral effect by binding to viral RNA through its CCCH zinc finger motif and recruiting host RNA exosome or cellular decapping complex to degrade viral RNA in the cytoplasm (Guo, Carroll et al, 2004;Lee, Komano et al, 2013). The ZAPresponsive elements (ZREs) vary among viral RNAs (Guo, Carroll et al, 2004;Zhu, Chen et al, 2011;Wang, Tu et al, 2012). Since there is no report of the effect of ZAP on enteroviruses infection and almost no biological function of ZAP has been confirmed in animal models of viral infection, it is of great interest to explore the possible antiviral function of ZAP on CVB3 and role of ZAP in the development of CVB3-induced acute viral myocarditis (VMC).…”

Zinc finger antiviral protein inhibits coxsackievirus B3 virus replication and protects against viral myocarditis

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