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在 SIV 和 HIV 感染期间,一组 CD14highCD16negCCR2low/neg 单核细胞亚群的扩增,其功能类似于髓系来源的抑制细胞。

Expansion of a subset of CD14highCD16negCCR2low/neg monocytes functionally similar to myeloid-derived suppressor cells during SIV and HIV infection.

机构信息

Johns Hopkins University School of Medicine, BRB 831, Baltimore, MD 21287, USA.

出版信息

J Leukoc Biol. 2012 May;91(5):803-16. doi: 10.1189/jlb.1111579. Epub 2012 Feb 24.

Abstract

Monocytes have been categorized in three main subpopulations based on CD14 and CD16 surface expression. Classical monocytes express the CD14(++)CD16(-)CCR2(+) phenotype and migrate to inflammatory sites by quickly responding to CCL2 signaling. Here, we identified and characterized the expansion of a novel monocyte subset during HIV and SIV infection, which were undistinguishable from classical monocytes, based on CD14 and CD16 expression, but expressed significantly lower surface CCR2. Transcriptome analysis of sorted cells demonstrated that the CCR2(low/neg) cells are a distinct subpopulation and express lower levels of inflammatory cytokines and activation markers than their CCR2(high) counterparts. They exhibited impaired phagocytosis and greatly diminished chemotaxis in response to CCL2 and CCL7. In addition, these monocytes are refractory to SIV infection and suppress CD8(+) T cell proliferation in vitro. These cells express higher levels of STAT3 and NOS2, suggesting a phenotype similar to monocytic myeloid-derived cells, which suppress expansion of CD8(+) T cells in vivo. They may reflect an antiproliferative response against the extreme immune activation observed during HIV and SIV infections. In addition, they may suppress antiviral responses and thus, have a role in AIDS pathogenesis. Antiretroviral therapy in infected macaque and human subjects caused this population to decline, suggesting that this atypical phenotype is linked to viral replication.

摘要

根据 CD14 和 CD16 表面表达,单核细胞已被分为三个主要亚群。经典单核细胞表达 CD14(++)CD16(-)CCR2(+)表型,通过快速响应 CCL2 信号而迁移到炎症部位。在这里,我们在 HIV 和 SIV 感染期间鉴定并表征了一种新型单核细胞亚群的扩增,该亚群基于 CD14 和 CD16 表达与经典单核细胞无法区分,但表面 CCR2 的表达显著降低。分选细胞的转录组分析表明,CCR2(low/neg)细胞是一个独特的亚群,与 CCR2(high)细胞相比,其表达的炎症细胞因子和激活标志物水平较低。它们对 CCL2 和 CCL7 的吞噬作用受损,趋化性大大降低。此外,这些单核细胞对 SIV 感染具有抗性,并在体外抑制 CD8(+)T 细胞增殖。这些细胞表达更高水平的 STAT3 和 NOS2,表明其表型类似于单核细胞髓样来源细胞,可在体内抑制 CD8(+)T 细胞的扩增。它们可能反映了针对 HIV 和 SIV 感染期间观察到的极端免疫激活的抗增殖反应。此外,它们可能抑制抗病毒反应,从而在艾滋病发病机制中发挥作用。感染猴和人类接受抗逆转录病毒治疗后,该群体数量下降,表明这种非典型表型与病毒复制有关。

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