Virus - EDK - BIG Data Center

Abbr: HCV
Classification: dsDNA
Protein Sequence: polyprotein; core protein; envelope protein E1; envelope protein E2; protein p7; nonstructural protein NS2; protease/helicase protein NS3; nonstructural protein NS4A; nonstructural protein NS4B; nonstructural protein NS5A; RNA-dependent RNA polymerase NS5B; protein F
Summary: APOBECs and ADAR enzyme inhibit HBV infection and replication

Virus	Host	Enzyme	Phenotype	Disease
Hepatitis C virus	Human	ADAR1	Inhibit viral replication	Hepatitis
Correlation: Negative Description: Small inhibitory RNA, specific for ADAR1, stimulated the replicon 40-fold, indicating that ADAR1 has a role in limiting replication of the viral RNA. PMID: 15858013
Hepatitis C virus	Human	APOBEC3G	Increased expression of the editing enzyme	Hepatitis
Correlation: Negative Description: Transfection of the NS5A gene, but not any other non-structural protein genes of HCV tested, to the hepatocellular carcinoma cell line enhanced APOBEC3G expression. PMID: 17036163
Hepatitis C virus	Human	APOBEC3G	Inhibit viral replication	Hepatitis
Correlation: Negative Description: Introduction of external hA3G into HCV-infected Huh7.5 human hepatocytes inhibited HCV replication; knockdown of endogenous hA3G enhanced HCV replication. Exogenous HIV-1 virion infec- tivity factor (Vif) decreased intracellular hA3G and therefore enhanced HCV proliferation, suggesting that the presence of Vif might be an explanation for the HIV-1/HCV coinfection often observed in HIV-1(1) individuals. PMID: 21480314
Hepatitis C virus	Human; Mice	APOBEC3	Antiviral	Hepatitis
Correlation: Negative Description: The researchers developed TCR-reprogrammed nonlytic T cells capable of activating APOBEC3 in hepatoma cells and in HBV-infected human hepatocytes in mice, limiting viral infection. These cells with limited hepatotoxicity might be developed for treatment of chronic HBV infection. PMID: 29550589
Hepatitis C virus	Human	APOBEC3	Antiviral	Hepatitis
Correlation: Negative Description: The virus produced by APOB KO cells had significantly diminished infectivity as measured by the TCID-50 method compared to wild-type virus. Lipidomic analysis demonstrated that these virions have a fundamentally altered lipidome, with complete depletion of cholesterol esters. We further demonstrate that inhibition of apoB using mipomersen, an FDA-approved anti-sense oligonucleotide, results in a potent anti-HCV effect and significantly reduces the infectivity of the virus. PMID: 28018102

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Hepatitis C virus - HCV