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载脂蛋白B胞苷脱氨酶对泡沫病毒的限制作用

Restriction of foamy viruses by APOBEC cytidine deaminases.

作者信息

Delebecque Frédéric, Suspène Rodolphe, Calattini Sara, Casartelli Nicoletta, Saïb Ali, Froment Alain, Wain-Hobson Simon, Gessain Antoine, Vartanian Jean-Pierre, Schwartz Olivier

机构信息

Virus and Immunity Group, URA CNRS 1930, Institut Pasteur, 75724 Paris cedex 15, France.

出版信息

J Virol. 2006 Jan;80(2):605-14. doi: 10.1128/JVI.80.2.605-614.2006.

Abstract

Foamy viruses (FVs) are nonpathogenic retroviruses infecting many species of mammals, notably primates, cattle, and cats. We have examined whether members of the apolipoprotein B-editing catalytic polypeptide-like subunit (APOBEC) family of antiviral cytidine deaminases restrict replication of simian FV. We show that human APOBEC3G is a potent inhibitor of FV infectivity in cell culture experiments. This antiviral activity is associated with cytidine editing of the viral genome. Both molecular FV clones and primary uncloned viruses were susceptible to APOBEC3G, and viral infectivity was also inhibited by murine and simian APOBEC3G homologues, as well as by human APOBEC3F. Wild-type and bet-deleted viruses were similarly sensitive to this antiviral activity, suggesting that Bet does not significantly counteract APOBEC proteins. Moreover, we did not detect FV sequences that may have been targeted by APOBEC in naturally infected macaques, but we observed a few G-to-A substitutions in humans that have been accidentally contaminated by simian FV. In infected hosts, the persistence strategy employed by FV might be based on low levels of replication, as well as avoidance of cells expressing large amounts of active cytidine deaminases.

摘要

泡沫病毒(FVs)是感染多种哺乳动物,尤其是灵长类动物、牛和猫的非致病性逆转录病毒。我们研究了抗病毒胞苷脱氨酶载脂蛋白B编辑催化多肽样亚基(APOBEC)家族成员是否限制猿猴泡沫病毒的复制。我们发现在细胞培养实验中,人APOBEC3G是FV感染性的有效抑制剂。这种抗病毒活性与病毒基因组的胞苷编辑有关。分子FV克隆和未克隆的原始病毒均对APOBEC3G敏感,并且鼠类和猿猴APOBEC3G同源物以及人APOBEC3F也抑制病毒感染性。野生型和缺失Bet的病毒对这种抗病毒活性同样敏感,这表明Bet不会显著对抗APOBEC蛋白。此外,我们在自然感染的猕猴中未检测到可能被APOBEC靶向的FV序列,但在被猿猴FV意外污染的人类中观察到一些G到A的替换。在受感染的宿主中,FV采用的持续存在策略可能基于低水平复制以及避开表达大量活性胞苷脱氨酶的细胞。

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