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在自然感染过程中 HIV-1 Rev 反应元件的进化揭示了随时间变化而改变结构和增加活性的核苷酸变化。

Evolution of the HIV-1 Rev Response Element during Natural Infection Reveals Nucleotide Changes That Correlate with Altered Structure and Increased Activity over Time.

机构信息

Basic Research Laboratory, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Frederick, Maryland, USA.

Division of Infectious Diseases and International Health, Department of Medicine, University of Virginia, Charlottesville, Virginia, USA.

出版信息

J Virol. 2019 May 15;93(11). doi: 10.1128/JVI.02102-18. Print 2019 Jun 1.

Abstract

The HIV-1 Rev response element (RRE) is a -acting RNA element characterized by multiple stem-loops. Binding and multimerization of the HIV Rev protein on the RRE promote the nucleocytoplasmic export of incompletely spliced mRNAs, an essential step in HIV replication. Most of our understanding of the Rev-RRE regulatory axis comes from studies of lab-adapted HIV clones. However, in human infection, HIV evolves rapidly, and mechanistic studies of naturally occurring Rev and RRE sequences are essential to understanding this system. We previously described the functional activity of two RREs found in circulating viruses in a patient followed during the course of HIV infection. The early RRE was less functionally active than the late RRE, despite differing in sequence by only 4 nucleotides. In this study, we describe the sequence, function, and structural evolution of circulating RREs in this patient using plasma samples collected over 6 years of untreated infection. RRE sequence diversity varied over the course of infection, with evidence of selection pressure that led to sequence convergence as disease progressed being found. An increase in RRE functional activity was observed over time, and a key mutation was identified that correlates with a major conformational change in the RRE and increased functional activity. Additional mutations were found that may have contributed to increased activity as a result of greater Shannon entropy in RRE stem-loop II, which is key to primary Rev binding. HIV-1 replication requires interaction of the viral Rev protein with a -acting regulatory RNA, the Rev response element (RRE), whose sequence changes over time during infection within a single host. In this study, we show that the RRE is subject to selection pressure and that RREs from later time points in infection tend to have higher functional activity. Differences in RRE functional activity are attributable to specific changes in RNA structure. Our results suggest that RRE evolution during infection may be important for HIV pathogenesis and that efforts to develop therapies acting on this viral pathway should take this into account.

摘要

HIV-1 反式激活因子(Rev)反应元件(RRE)是一种具有多个茎环结构的-作用 RNA 元件。HIV Rev 蛋白结合和多聚化在 RRE 上,促进了不完全剪接的 mRNA 的核质输出,这是 HIV 复制的一个关键步骤。我们对 Rev-RRE 调控轴的大部分了解都来自于对实验室适应的 HIV 克隆的研究。然而,在人类感染中,HIV 会迅速进化,对天然存在的 Rev 和 RRE 序列的机制研究对于理解这个系统至关重要。我们之前描述了在一名 HIV 感染者的循环病毒中发现的两个 RRE 的功能活性。尽管早期 RRE 的序列仅相差 4 个核苷酸,但它的功能活性却比晚期 RRE 差。在这项研究中,我们使用未经治疗的感染 6 年期间采集的血浆样本,描述了该患者循环 RRE 的序列、功能和结构进化。感染过程中 RRE 序列多样性发生了变化,发现了选择压力的证据,导致随着疾病的进展序列趋同。随着时间的推移,RRE 的功能活性增加,并且确定了一个关键突变,该突变与 RRE 中主要构象变化和功能活性增加相关。还发现了其他突变,由于 RRE 茎环 II 的 Shannon 熵增加,可能导致功能活性增加,这是 Rev 结合的关键。HIV-1 复制需要病毒 Rev 蛋白与-作用调节 RNA(Rev 反应元件,RRE)相互作用,其序列在单个宿主内的感染过程中随时间而变化。在这项研究中,我们表明 RRE 受到选择压力的影响,并且感染后期时间点的 RRE 往往具有更高的功能活性。RRE 功能活性的差异归因于 RNA 结构的特定变化。我们的研究结果表明,感染过程中 RRE 的进化可能对 HIV 发病机制很重要,并且应该考虑针对该病毒途径的治疗方法。

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