Antiviral Effect of Interferon-Induced Guanylate Binding Protein-1 against Coxsackie Virus and Hepatitis B Virus B3 in Vitro

被引:7
作者
Yinping LUBaoju WANGJihua DONGZhao LIUShihe GUANMengji LU and Dongliang YANGDepartment of VirologyUnion Hospital of Tongji Medical CollegeHuazhong University of Science and TechnologyWuhan ChinaDivision of Clinical ImmunologyTongji Hospital of Tongji Medical CollegeHuazhong University of Science and TechnologyWuhan ChinaInstitute of VirologyDuisburgEssen UniversityEssen Germany [1 ,2 ,2 ,1 ,1 ,3 ,3 ,2 ,1 ,430022 ,2 ,430030 ,3 ,45147 ]
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R96 [药理学];
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100706 [药理学];
摘要
Guanylate binding protein-1(GBP-1)is an interferon-induced protein.To observe its antiviral effect against Hepatitis B virus(HBV)and Coxsackie virus B3(CVB3),we constructed an eukaryotic expression vector of human GBP-1(hGBP-1).Full-length encoding sequence of hGBP-1 was amplified by long chain RT-PCR and inserted into a pCR2.1 vector,then subcloned into a pCDNA3.1(-)vector.Recombinant hGBP-1 plasmids and pHBV1.3 carrying 1.3-fold genome of HBV were contransfected into HepG2 cells,and inhibition effect of hGBP-1 against HBV replication was observed.Hela cells transfected with recombinant hGBP-1 plasmids were challenged with CVB3,and viral yield in cultures were detected.The results indicated that recombinant eukaryotic expression plasmid of hGBP-1 was constructed successfully and the hGBP-1 gene carried in this plasmid could be efficiently expressed in HepG2 cells and Hela cells.hGBP-1 inhibit CVB3 but not HBV replication in vitro.These results demonstrate that hGBP-1 mediates an antiviral effect against CVB3 but not HBV and perhaps plays an important role in the interferon-mediated antiviral response against CVB3.
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页码:193 / 198
页数:6
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