首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Proteasome inhibitors uncouple rhesus TRIM5 alpha restriction of HIV-1 reverse transcription and infection
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Proteasome inhibitors uncouple rhesus TRIM5 alpha restriction of HIV-1 reverse transcription and infection

机译:蛋白酶体抑制剂解耦恒河猴TRIM5α限制HIV-1逆转录和感染

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摘要

The primate TRIM5 alpha proteins have recently been defined as cellular restriction factors, preventing primate infection by retroviruses from different species. For instance, rhesus TRIM5 alpha (rhTRIM5 alpha) restricts infection by HIV-1. Virtually all TRIM5a proteins block the early replication of retroviruses by preventing the accumulation of reverse transcription products, but the underlying mechanism remains unclear. In this article, we find that disrupting proteasome function alters rhTRIM5 alpha localization and allows the normal generation of HIV-1 late reverse transcription products, even though HIV-1 infection and the generation of nuclear 1-LTR and 2-LTR viral cDNA forms remain impaired. This finding suggests rhTRIM5 alpha restricts HIV infection in two distinct phases: (i) altering the normal passage of the reverse-transcribing viral genome to the nucleus and (ii) targeting the reverse transcription complex to be disrupted by the proteasome. Because proteasome inhibitor blocks the second phase, accumulation of a nonfunctional viral DNA genome can be readily observed. Defining each phase may reveal HIV-1 targets for future antiviral therapy in which dual blockade may be equally as effective as naturally occurring rhTRIM5 alpha protein in preventing HIV-1 infection in vivo.
机译:灵长类动物TRIM5α蛋白最近已被定义为细胞限制性因子,可防止不同物种的逆转录病毒感染灵长类动物。例如,恒河猴TRIM5 alpha(rhTRIM5 alpha)限制了HIV-1的感染。实际上,所有TRIM5a蛋白都通过阻止逆转录产物的积累来阻止逆转录病毒的早期复制,但是其潜在机制仍不清楚。在本文中,我们发现破坏蛋白酶体功能会改变rhTRIM5 alpha的定位,并允许正常产生HIV-1晚期逆转录产物,即使仍然存在HIV-1感染以及核LTR和2-LTR病毒cDNA形式的产生受损。这一发现表明,rhTRIM5 alpha在两个不同的阶段限制了HIV的感染:(i)改变逆转录病毒基因组向核的正常传递,以及(ii)靶向逆转录复合物被蛋白酶体破坏。因为蛋白酶体抑制剂阻断了第二阶段,所以很容易观察到无功能的病毒DNA基因组的积累。定义每个阶段可能会揭示HIV-1靶点,以用于将来的抗病毒治疗,其中双重阻断在体内预防HIV-1感染方面可能与天然存在的rhTRIM5α蛋白同样有效。

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