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Dynamic Perturbations of the T-Cell Receptor Repertoire in Chronic HIV Infection and following Antiretroviral Therapy

机译:慢性HIV感染和抗逆转录病毒治疗后T细胞受体库的动态扰动

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摘要

HIV infection profoundly affects many parameters of the immune system and ultimately leads to AIDS, yet which factors are most important for determining resistance, pathology, and response to antiretroviral treatment – and how best to monitor them – remain unclear. We develop a quantitative high-throughput sequencing pipeline to characterize the TCR repertoires of HIV-infected individuals before and after antiretroviral therapy, working from small, unfractionated samples of peripheral blood. This reveals the TCR repertoires of HIV+ individuals to be highly perturbed, with considerably reduced diversity as a small proportion of sequences are highly overrepresented. HIV also causes specific qualitative changes to the repertoire including an altered distribution of V gene usage, depletion of public TCR sequences, and disruption of TCR networks. Short-term antiretroviral therapy has little impact on most of the global damage to repertoire structure, but is accompanied by rapid changes in the abundance of many individual TCR sequences, decreases in abundance of the most common sequences, and decreases in the majority of HIV-associated CDR3 sequences. Thus, high-throughput repertoire sequencing of small blood samples that are easy to take, store, and process can shed light on various aspects of the T-cell immune compartment and stands to offer insights into patient stratification and immune reconstitution.
机译:HIV感染会深刻影响免疫系统的许多参数,最终导致AIDS,然而,尚不清楚哪些因素对于确定耐药性,病理学和对抗逆转录病毒疗法的反应(以及如何对其进行最佳监测)最为重要。我们开发了定量高通量测序管线,以表征抗逆转录病毒治疗前后HIV感染者的TCR组成,该研究使用少量的普通血液样本进行。这表明HIV + 个体的TCR谱表受到高度干扰,多样性显着降低,因为一小部分序列被高度代表。 HIV还导致库的特定质变,包括V基因使用情况的变化,公共TCR序列的消耗以及TCR网络的破坏。短期抗逆转录病毒疗法对所有整体库结构的破坏几乎没有影响,但伴随着许多单个TCR序列丰度的快速变化,最常见序列的丰度降低,而大多数HIV-相关的CDR3序列。因此,易于采集,存储和处理的小血样的高通量库测序可以阐明T细胞免疫区室的各个方面,并为深入了解患者分层和免疫重建提供依据。

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