首页> 外文OA文献 >Determination of antigen-specific memory/effector CD4+ T cell frequencies by flow cytometry: evidence for a novel, antigen-specific homeostatic mechanism in HIV-associated immunodeficiency.
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Determination of antigen-specific memory/effector CD4+ T cell frequencies by flow cytometry: evidence for a novel, antigen-specific homeostatic mechanism in HIV-associated immunodeficiency.

机译:通过流式细胞术确定抗原特异性记忆/效应CD4 + T细胞的频率:HIV相关免疫缺陷的新型,抗原特异性稳态机制的证据。

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摘要

The highly regulated secretion of effector cytokines by CD4+ T cells plays a critical role in immune protection against pathogens such as cytomegalovirus. Here, we directly compare the frequency and functional characteristics of cytomegalovirus-specific CD4+ memory/effector T cells in normal and HIV+ subjects using a novel, highly efficient multiparameter flow cytometric assay that detects the rapid intracellular accumulation of cytokine(s) after short-term (6 h) in vitro antigen stimulation. Responses in this assay correlate precisely with independent measures of sensitization history (e.g., seroreactivity), and allow the simultaneous assessment of multiple cytokines in single effector T cells. Healthy HIV- individuals manifested an average of 0.71, 0.72, 0.38, and 0.06% CD4+ T cells responding to cytomegalovirus with gamma-IFN, TNF-alpha, IL-2, and IL-4 production, respectively, with the simultaneous production of gamma-IFN, TNF-alpha, and IL-2 being the most common effector phenotype. Significantly, overall cytomegalovirus-specific CD4+ effector frequencies were markedly higher among 40% of HIV+ subjects (2.7-8.0%), and demonstrated a predominately polarized gamma-IFN+/TNF-alpha+/IL-2-/IL-4- phenotype. In contrast, CD4+ effector frequencies for heterologous, nonubiquitous viruses such as the mumps virus were low or absent in the HIV+ group. These data suggest the existence of homeostatic mechanisms in HIV disease that selectively preserve memory T cell populations reactive with ubiquitous pathogens such as cytomegalovirus-likely at the expense of T cell memory to more sporadically encountered infectious agents.
机译:CD4 + T细胞对效应细胞因子分泌的高度调控在针对病原体(如巨细胞病毒)的免疫保护中起着至关重要的作用。在这里,我们使用新颖,高效的多参数流式细胞术检测,可在短期内检测细胞因子的快速细胞内蓄积,从而直接比较正常人和HIV +受试者中巨细胞病毒特异的CD4 +记忆/效应T细胞的频率和功能特征(6小时)体外抗原刺激。该测定法中的反应与致敏史的独立测量值(例如血清反应性)精确相关,并允许同时评估单个效应T细胞中的多种细胞因子。健康的HIV个体表现出平均0.71、0.72、0.38和0.06%的CD4 + T细胞对巨细胞病毒的反应,分别产生γ-IFN,TNF-α,IL-2和IL-4,同时产生γ -IFN,TNF-α和IL-2是最常见的效应表型。值得注意的是,在40%的HIV +受试者中(2.7-8.0%),总的巨细胞病毒特异性CD4 +效应子频率显着更高,并且表现出主要极化的γ-IFN+ /TNF-α+ / IL-2- / IL-4-表型。相比之下,HIV +组中异源性,无处不在的病毒(例如腮腺炎病毒)的CD4 +效应子频率低或不存在。这些数据表明,在HIV疾病中存在稳态机制,该机制可以选择性地保留与普遍存在的病原体(例如巨细胞病毒)反应的记忆T细胞种群,而可能以牺牲T细胞记忆为代价,使偶发性传染病传染。

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