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CD27?CD38 B cells accumulated in early HIV infection exhibit transitional profile and promote HIV disease progression

机译:CD27?CD38 B细胞在早期HIV感染中累积,表现出过渡性外形并促进艾滋病毒疾病进展

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Although peripheral B cell dysfunction in early HIV infection is established, how B cell subsets are altered by HIV infection is poorly understood. While investigating B cell subsets among individuals recently infected with HIV, we observe an accumulation of CD27 ? CD38 B cells and find that these cells can directly facilitate HIV infection of primary CD4 T?cells in?vitro . Comprehensive analyses of the phenotype, function, and transcriptome of the CD27 ? CD38 B cell subset is conducted compared with memory and naive B cells. We find that the CD27 ? CD38 B cells exhibit a transitional B cell phenotype and an extremely high turnover rate. Importantly, individuals with higher proportions of CD27 ? CD38 B cells during early HIV infection tend to become rapid progressors in the chronic infection stage. In this study, we identify a peripheral transitional B cell subset that accumulates during early HIV infection and may contribute to disease progression.
机译:虽然建立了早期艾滋病毒感染的外周B细胞功能障碍,但如何通过HIV感染改变B细胞亚群的变化很差。 在最近感染艾滋病毒的个体中调查B细胞亚群,我们观察CD27的积累? CD38 B细胞并发现这些细胞可以直接促进艾滋病毒感染原发性CD4T≥细胞的体外细胞。 CD27的表型,功能和转录组综合分析? 与记忆和幼稚B细胞进行比较CD38b细胞子集。 我们发现CD27? CD38 B细胞表现出过渡性B细胞表型和极高的周转率。 重要的是,具有更高比例的CD27的个人? 艾滋病毒过早感染期间CD38 B细胞往往成为慢性感染阶段的快速进展。 在本研究中,我们鉴定了在早期艾滋病毒感染期间积累的外周过渡性B细胞亚集,并且可能有助于疾病进展。

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