首页> 美国卫生研究院文献>Journal of Virology >Differential Restriction of Human Immunodeficiency Virus Type 2 and Simian Immunodeficiency Virus SIVmac by TRIM5α Alleles
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Differential Restriction of Human Immunodeficiency Virus Type 2 and Simian Immunodeficiency Virus SIVmac by TRIM5α Alleles

机译:TRIM5α等位基因对2型人类免疫缺陷病毒和猿猴免疫缺陷病毒SIVmac的差异性限制

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摘要

Primate lentiviruses have narrow host ranges, due in part to their sensitivities to mammalian intracellular antiviral factors such as APOBEC3G and TRIM5α. Despite the protection provided by this innate immune system, retroviruses are able to transfer between species where they can cause disease. This is true for sooty mangabey simian immunodeficiency virus, which has transferred to humans as HIV-2 and to rhesus macaques as SIVmac, where it causes AIDS. Here we examine the sensitivities of the closely related HIV-2 and SIVmac to restriction by TRIM5α. We show that rhesus TRIM5α can restrict HIV-2 but not the closely related SIVmac. SIVmac has not completely escaped TRIM5α, as shown by its sensitivity to distantly related TRIM5α from the New World squirrel monkey. Squirrel monkey TRIM5α blocks SIVmac infection after DNA synthesis and is not saturable with restriction-sensitive virus-like particles. We map the determinant for TRIM5α sensitivity to the structure in the capsid protein that recruits CypA into HIV-1 virions. We also make an SIV, mutated at this site, which bypasses restriction in all cells tested.
机译:灵长类慢病毒宿主范围狭窄,部分是由于它们对哺乳动物细胞内抗病毒因子(如APOBEC3G和TRIM5α)的敏感性。尽管先天免疫系统提供了保护,但逆转录病毒仍能够在可能引起疾病的物种之间转移。乌黑的猿猴猿免疫缺陷病毒确实如此,它已经以HIV-2的形式传播给人类,并以SIVmac的形式传播到了恒河猴,从而引起了艾滋病。在这里,我们检查了密切相关的HIV-2和SIVmac对TRIM5α限制的敏感性。我们显示恒河猴TRIM5α可以限制HIV-2,但不能限制紧密相关的SIVmac。 SIVmac尚未完全摆脱TRIM5α,正如它对来自新大陆松鼠猴的远缘TRIM5α的敏感性所表明的那样。松鼠猴TRIM5α可以在DNA合成后阻止SIVmac感染,并且不能被限制敏感的病毒样颗粒所饱和。我们将TRIM5α敏感性的决定因素映射到将CypA募集到HIV-1病毒体的衣壳蛋白中的结构上。我们还制作了一个在该位点突变的SIV,它绕过了所有测试细胞的限制。

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