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RNA helicase A modulates translation of HIV-1 and infectivity of progeny virions.

机译:RNA解旋酶A调节HIV-1的翻译和子代病毒体的感染性。

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摘要

Retroviruses rely on host RNA-binding proteins to modulate various steps in their replication. Previously several animal retroviruses were determined to mediate Dhx9/RNA helicase A (RHA) interaction with a 5' terminal post-transcriptional control element (PCE) for efficient translation. Herein PCE reporter assays determined HTLV-1 and HIV-1 RU5 confer orientation-dependent PCE activity. The effect of Dhx9/RHA down-regulation and rescue with siRNA-resistant RHA on expression of HIV-1NLtpd provirus determined that RHA is necessary for efficient HIV-1 RNA translation and requires ATPase-dependent helicase function. Quantitative analysis determined HIV-1 RNA steady-state and cytoplasmic accumulation were not reduced; rather the translational activity of viral RNA was reduced. Western blotting determined that RHA-deficient virions assemble with Lys-tRNA synthetase, exhibit processed reverse transcriptase and contain similar level of viral RNA, but they are poorly infectious on primary lymphocytes and HeLa cells. The results demonstrate RHA is an important host factor within the virus-producer cell and within the viral particle. The identification of RHA-dependent PCE activity in cellular junD RNA and in six of seven genera of Retroviridae suggests conservation of this translational control mechanism among vertebrates, and convergent evolution of Retroviridae to utilize this host mechanism.
机译:逆转录病毒依赖于宿主RNA结合蛋白来调节其复制中的各个步骤。以前,已经确定了几种动物逆转录病毒来介导Dhx9 / RNA解旋酶A(RHA)与5'末端转录后控制元件(PCE)的相互作用,以进行有效翻译。本文中,PCE记者测定法确定了HTLV-1和HIV-1 RU5赋予了方向依赖性PCE活性。 Dhx9 / RHA下调和用siRNA抗性RHA拯救对HIV-1NLtpd前病毒表达的影响确定RHA是有效HIV-1 RNA翻译所必需的,并且需要ATPase依赖性解旋酶功能。定量分析确定HIV-1 RNA的稳态和细胞质的积累没有减少。而是病毒RNA的翻译活性降低了。 Western印迹法检测到,缺乏RHA的病毒粒子与Lys-tRNA合成酶组装在一起,表现出加工的逆转录酶并含有相似水平的病毒RNA,但它们对原代淋巴细胞和HeLa细胞的感染力较弱。结果表明,RHA是病毒生产细胞内和病毒颗粒内的重要宿主因子。在细胞junD RNA和逆转录病毒科的七个属中的六个中鉴定出RHA依赖的PCE活性,表明了脊椎动物之间这种翻译控制机制的保守性,以及逆转录病毒科利用该宿主机制的趋同进化。

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