Antiviral Warrior—APOBEC3G

Antiviral Warrior—APOBEC3G

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摘要 This paper is to further understand how APOBEC3G can defend the retroviruses and to find new approaches to AIDs （acquired immure deficiency syndrome）.The viral infectivity factor （Vif） induces rapid degradation of APOBEC3G by ubiquitination, which is a proteosome-dependent pathway. Precisely speaking, only in the virus-producing cell Vif expression is necessary; in its absence, infection of a subsequent target cell terminates at a postentry step through the action of the human APOBEC3G antiviral mechanism. Hf protein has two domains： one binds to APOBEC3G and the other regulates the degradation of APOBEC3G by a conserved sequence, SLQ （Y/F） LA motif. Recently, the research on Vif has also revealed APOBEC3G is a novel component of innate immune system. In fact, APOBEC3G not only acts in DNA editing to block the replication of retroviruses such as HIV-1, but also is able to defend a wide spectrum of distantly related retroviruses and interferes with HBV through a different mechanism from HIE. This paper is to further understand how APOBEC3G can defend the retroviruses and to find new approaches to AIDs （acquired immure deficiency syndrome）.The viral infectivity factor （Vif） induces rapid degradation of APOBEC3G by ubiquitination, which is a proteosome-dependent pathway. Precisely speaking, only in the virus-producing cell Vif expression is necessary; in its absence, infection of a subsequent target cell terminates at a postentry step through the action of the human APOBEC3G antiviral mechanism. Hf protein has two domains： one binds to APOBEC3G and the other regulates the degradation of APOBEC3G by a conserved sequence, SLQ （Y/F） LA motif. Recently, the research on Vif has also revealed APOBEC3G is a novel component of innate immune system. In fact, APOBEC3G not only acts in DNA editing to block the replication of retroviruses such as HIV-1, but also is able to defend a wide spectrum of distantly related retroviruses and interferes with HBV through a different mechanism from HIE.

作者吴小霞马义才

机构地区 School of life science and technology

出处《Journal of Electronic Science and Technology of China》 2005年第4期372-376,共5页 中国电子科技（英文版）

基金 the Cultivating Funds of Academic and Technical Leaders in Sichuan Province (No. 2200338)

关键词 HIV-1 CEM15/APOBEC3G VIF HYPERMUTATION innate immunity HBV HIV-1 CEM15/APOBEC3G Vif hypermutation innate immunity HBV

分类号 R512.91 [医药卫生—内科学]

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Journal of Electronic Science and Technology of China

2005年第4期

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