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A Novel Single-Cell FISH-Flow Assay Identifies Effector Memory CD4 + T cells as a Major Niche for HIV-1 Transcription in HIV-Infected Patients

机译:一种新型的单细胞FISH流测定法可确定效应记忆CD4 + T细胞是HIV感染患者HIV-1转录的主要利基。

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ABSTRACT Cells that actively transcribe HIV-1 have been defined as the “active viral reservoir” in HIV-infected individuals. However, important technical limitations have precluded the characterization of this specific viral reservoir during both treated and untreated HIV-1 infections. Here, we used a novel single-cell RNA fluorescence in situ hybridization-flow cytometry (FISH-flow) assay that requires only 15 million unfractionated peripheral blood mononuclear cells (PBMCs) to characterize the specific cell subpopulations that transcribe HIV RNA in different subsets of CD4~(+)T cells. In samples from treated and untreated HIV-infected patients, effector memory CD4~(+)T cells were the main cell population supporting HIV RNA transcription. The number of cells expressing HIV correlated with the plasma viral load, intracellular HIV RNA, and proviral DNA quantified by conventional methods and inversely correlated with the CD4~(+)T cell count and the CD4/CD8 ratio. We also found that after ex vivo infection of unstimulated PBMCs, HIV-infected T cells upregulated the expression of CD32. In addition, this new methodology detected increased numbers of primary cells expressing viral transcripts and proteins after ex vivo viral reactivation with latency reversal agents. This RNA FISH-flow technique allows the identification of the specific cell subpopulations that support viral transcription in HIV-1-infected individuals and has the potential to provide important information on the mechanisms of viral pathogenesis, HIV persistence, and viral reactivation. IMPORTANCE Persons infected with HIV-1 contain several cellular viral reservoirs that preclude the complete eradication of the viral infection. Using a novel methodology, we identified effector memory CD4~(+)T cells, immune cells preferentially located in inflamed tissues with potent activity against pathogens, as the main cells encompassing the transcriptionally active HIV-1 reservoir in patients on antiretroviral therapy. Importantly, the identification of such cells provides us with an important target for new therapies designed to target the hidden virus and thus to eliminate the virus from the human body. In addition, because of its ability to identify cells forming part of the viral reservoir, the assay used in this study represents an important new tool in the field of HIV pathogenesis and viral persistence.
机译:摘要主动转录HIV-1的细胞已被定义为感染HIV的个体的“活跃病毒库”。但是,重要的技术限制使得在治疗和未治疗的HIV-1感染期间都无法确定这种特定病毒库的特征。在这里,我们使用了一种新颖的单细胞RNA荧光原位杂交流式细胞术(FISH-flow)分析,仅需要1500万未分级的外周血单核细胞(PBMC)来表征在不同亚群中转录HIV RNA的特定细胞亚群。 CD4〜(+)T细胞在已治疗和未治疗的HIV感染患者的样本中,效应记忆CD4〜(+)T细胞是支持HIV RNA转录的主要细胞群。表达HIV的细胞数量与血浆病毒载量,细胞内HIV RNA和原病毒DNA数量相关,而这些数量是通过常规方法量化的,与CD4〜(+)T细胞计数和CD4 / CD8比值呈负相关。我们还发现,离体感染未刺激的PBMC后,HIV感染的T细胞会上调CD32的表达。另外,在用潜伏期逆转剂进行离体病毒激活后,这种新方法检测出表达病毒转录本和蛋白质的原代细胞数量增加。这种RNA FISH-flow技术可鉴定支持HIV-1感染者中病毒转录的特定细胞亚群,并具有提供有关病毒发病机理,HIV持久性和病毒再激活机制的重要信息的潜力。重要信息感染HIV-1的人含有几个细胞病毒库,无法完全根除病毒感染。使用一种新颖的方法,我们确定了效应记忆CD4〜(+)T细胞(免疫细胞优先位于发炎的组织中,具有对病原体的强大活性),是包含抗逆转录病毒疗法患者转录活性HIV-1储库的主要细胞。重要的是,这些细胞的鉴定为我们提供了一种新的重要靶标,旨在针对隐性病毒从而从人体清除病毒的新疗法。另外,由于其能够鉴定构成病毒库一部分的细胞的能力,本研究中使用的测定方法代表了HIV发病机理和病毒持久性领域的重要新工具。

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