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逃过人及恒河猴 TRIM5α 的鼠白血病病毒的比较。

A comparison of murine leukemia viruses that escape from human and rhesus macaque TRIM5αs.

机构信息

Division of Virology, MRC National Institute for Medical Research, Mill Hill, London, United Kingdom.

出版信息

J Virol. 2013 Jun;87(11):6455-68. doi: 10.1128/JVI.03425-12. Epub 2013 Mar 27.

Abstract

To better understand the binding mechanism of TRIM5α to retrovirus capsid, we had previously selected N-tropic murine leukemia virus (N-MLV) mutants escaping from rhesus macaque TRIM5α (rhTRIM5α) by passaging the virus in rhTRIM5α-expressing cells and selecting for nonrestricted variants. To test the commonality of the findings from the rhTRIM5α study, we have now employed a similar genetic approach using human TRIM5α (huTRIM5α). Consistent with the rhTRIM5α study, the mapped huTRIM5α escape mutations were distributed across the capsid exterior, confirming the extended binding surface between virus and restriction factor. Compared to the results of the previous study, fewer escape mutations were identified, with particular mutants being repeatedly selected. Three out four huTRIM5α escape variants showed resistance to all primate TRIM5αs tested, but two of them sacrificed viral fitness, observations that were not made in the rhTRIM5α study. Moreover, differences in amino acid changes associated with escape from hu- and rhTRIM5αs suggested a charge dependence of the restriction by different TRIM5αs. Taken together, these results suggest that the recognition of the entire capsid surface is a general strategy for TRIM5α to restrict MLV but that significantly different specific interactions are involved in the binding of TRIM5α from different species to the MLV capsid core.

摘要

为了更好地理解 TRIM5α 与逆转录病毒衣壳的结合机制,我们之前通过在表达 rhTRIM5α 的细胞中传代病毒并选择不受限制的变体,从恒河猴 TRIM5α(rhTRIM5α)中筛选出逃避灵长类动物 TRIM5α(rhTRIM5α)的 N 型嗜性鼠白血病病毒(N-MLV)突变体。为了测试 rhTRIM5α 研究结果的普遍性,我们现在使用类似的遗传方法,使用人 TRIM5α(huTRIM5α)。与 rhTRIM5α 研究一致,映射的 huTRIM5α 逃逸突变分布在衣壳外部,证实了病毒和限制因子之间的扩展结合表面。与之前的研究结果相比,鉴定出的逃逸突变较少,特别是某些突变体被反复选择。四个 huTRIM5α 逃逸变体中有三个对所有测试的灵长类 TRIM5α 都表现出抗性,但其中两个牺牲了病毒的适应性,这在 rhTRIM5α 研究中没有观察到。此外,逃避 hu-和 rhTRIM5α 的氨基酸变化差异表明不同 TRIM5α 限制的电荷依赖性。总之,这些结果表明,识别整个衣壳表面是 TRIM5α 限制 MLV 的一般策略,但不同物种的 TRIM5α 与 MLV 衣壳核心结合涉及明显不同的特定相互作用。

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