The CD8 +HLA-DR + T cells expanded in HIV-1 infection are qualitatively identical to those from healthy controls

ImamichiH.; LempickiR.A.; AdelsbergerJ.W.HasleyR.B.RosenbergA.RobyG.RehmC.A.NelsonA.KrishnanS.PavlickM.WoodsC.J.BaselerM.W.LaneH.C.

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The CD8 +HLA-DR + T cells expanded in HIV-1 infection are qualitatively identical to those from healthy controls

机译：CD8 + HLA-DR + T细胞扩大hiv - 1这些感染定性是相同的从健康对照组

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HIV-induced immune activation leads to expansion of a subset of human CD8 + T cells expressing HLA-DR antigens. Expansion of CD8 +HLA-DR + T cells can be also observed in non-HIV settings including several autoimmune diseases and aging. Although these cells are felt to represent "immune exhaustion" and/or to be anergic, their precise role in host defense has remained unclear. Here, we report that this subset of cells exhibits a restricted repertoire, shows evidence of multiple rounds of division, but lacks markers of recent TCR engagement. Detailed cell cycle analysis revealed that compared with their CD8 +HLA-DR - counterpart, the CD8 +HLA-DR + T-cell pool contained an increased fraction of cells in S-phase with elevated levels of the G2/M regulators: cyclin A2, CDC25C, Cdc2 (CDK1), indicating that these cells are not truly anergic but rather experiencing proliferation in vivo. Together, these data support a hypothesis that antigen stimulation leads to the initial expansion of a CD8 + pool of cells in vivo that undergo further expansion independent of ongoing TCR engagement. No qualitative differences were noted between CD8 +HLA-DR + cells from HIV + and HIV - donors, indicating that the generation of CD8 +HLA-DR + T cells is a part of normal immune regulation that is exaggerated in the setting of HIV-1 infection.

机译：艾滋病病毒导致的免疫激活导致扩张一个子集的CD8 + T细胞表达HLA-DR抗原。细胞也可以观察到non-HIV设置包括一些自身免疫性疾病和衰老。虽然这些细胞感觉来表示“免疫疲劳”和/或无能,他们的在宿主防御仍然准确的作用不清楚。细胞表现出一种限制,节目多次分裂的证据,但是缺乏最近的标记细胞。细胞周期分析显示,相比之下CD8 + HLA-DR -同行,CD8 + HLA-DR+ t细胞池中增加的一部分细胞与高浓度的G2 / M s阶段监管机构:细胞周期蛋白A2、CDC25C Cdc2 (CDK1),这表明这些细胞并非真正的无能而是经历体内增殖。在一起,这些数据支持这一假说抗原刺激导致的初始扩张的CD8 +细胞体内进行独立的进一步扩张细胞受体。指出从HIV +和CD8 + HLA-DR +细胞之间艾滋病毒——捐助者,表明的生成CD8 + HLA-DR + T细胞是一种正常的免疫系统的一部分监管的设置被夸大了hiv - 1感染。

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《European Journal of Immunology》 |2012年第10期|2608-2620|共13页
作者
ImamichiH.; LempickiR.A.; AdelsbergerJ.W.HasleyR.B.RosenbergA.RobyG.RehmC.A.NelsonA.KrishnanS.PavlickM.WoodsC.J.BaselerM.W.LaneH.C.;
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作者单位

Clinical and Molecular Retrovirology Section, Laboratory of Immunoregulation, National Institute of;

Clinical Monitoring Research Program, Clinical Research Directorate, SAIC-Frederick, Inc.,;

Washington Hospital Center, Washington, DC, United StatesClinical Services Program, Applied/Developmental Research Directorate, SAIC-Frederick, Inc.,;

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原文格式 PDF
正文语种英语
中图分类医学免疫学;
关键词
host defense; Cell Cycle; HIVT-LymphocytesCD8 antigenHLA-DR AntigensHIV-1;

机译：宿主防御;细胞周期;HIVT-LymphocytesCD8;

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The CD8 +HLA-DR + T cells expanded in HIV-1 infection are qualitatively identical to those from healthy controls

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