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Leveraging Novel Integrated Single-Cell Analyses to Define HIV-1 Latency Reversal

机译:利用新型集成单细胞分析来定义HIV-1延迟逆转

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摘要

While suppressive antiretroviral therapy can effectively limit HIV-1 replication and evolution, it leaves behind a residual pool of integrated viral genomes that persist in a state of reversible nonproductive infection, referred to as the HIV-1 reservoir. HIV-1 infection models were established to investigate HIV-1 latency and its reversal; recent work began to probe the dynamics of HIV-1 latency reversal at single-cell resolution. Signals that establish HIV-1 latency and govern its reactivation are complex and may not be completely resolved at the cellular and regulatory levels by the aggregated measurements of bulk cellular-sequencing methods. High-throughput single-cell technologies that characterize and quantify changes to the epigenome, transcriptome, and proteome continue to rapidly evolve. Combinations of single-cell techniques, in conjunction with novel computational approaches to analyze these data, were developed and provide an opportunity to improve the resolution of the heterogeneity that may exist in HIV-1 reactivation. In this review, we summarize the published single-cell HIV-1 transcriptomic work and explore how cutting-edge advances in single-cell techniques and integrative data-analysis tools may be leveraged to define the mechanisms that control the reversal of HIV-1 latency.
机译:抑制抗逆转录病毒治疗可以有效地限制HIV-1复制和进化,但它留下了持续存在于可逆的非生产性感染状态的综合病毒基因组的残余池后面,称为HIV-1储层。建立了HIV-1感染模型,以调查HIV-1潜伏期及其逆转;最近的工作开始在单细胞分辨率下探测HIV-1潜伏逆转的动态。建立HIV-1潜伏期并控制其再激活的信号是复杂的,并且可以通过批量细胞测序方法的聚集测量来在细胞和调节水平上完全解决。高吞吐量单细胞技术,表征和量化对外延蛋白组,转录组和蛋白质组的变化继续迅速发展。开发了单细胞技术的组合,结合新颖的计算方法来分析这些数据,并提供有机会改善HIV-1重新激活中可能存在的异质性的分辨率。在本综述中,我们总结了已发表的单细胞HIV-1转录组作品,并探讨了单细胞技术的前沿进步和集成数据分析工具的方式如何利用来定义控制HIV-1潜伏期的逆转的机制。

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