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来自正常供体和HIV感染患者的CD4+CD7-辅助性T细胞的Th0/Th2样功能。

A Th0/Th2-like function of CD4+CD7- T helper cells from normal donors and HIV-infected patients.

作者信息

Autran B, Legac E, Blanc C, Debré P

机构信息

Laboratory of Cellular and Tissue Immunology, CNRS URA625, Hospital Pitié-Salpétrière, Paris, France.

出版信息

J Immunol. 1995 Feb 1;154(3):1408-17.

PMID:7529803
Abstract

We previously reported the expansion during HIV infection of a subset of CD4+ T cells characterized by a lack of CD7 cell surface expression. This CD4+CD7- subset showed in normal donors a lower cell proliferation than CD4+CD7+ autologous cells after CD3 triggering or CD28 costimulation. Our aim was to further characterize the Th function of this CD4+CD7- T cell subset, both in normal donors and in HIV-infected patients. Their CD4+CD7- cell proliferation and cytokine secretion were analyzed after cell-sorting and co-stimulation of the CD3 and CD28 pathways. In normal donors, the IL-2 produced by CD4+CD7- cells in response to a CD3 plus CD28 costimulus represented 50 +/- 28% of the autologous CD4+CD7+ cell IL-2 secretion. In addition, the CD4+CD7+ T cells produced higher amounts of IL-4 and IL-10 than the CD4+CD7+ cells with mean CD4+CD7-: CD4+CD7+ ratios of 5.4 +/- 4.5 and 26 +/- 25, for IL-4 and IL-10, respectively, whereas the IFN-gamma production was similar in both subsets. After a triggering of the CD3 complex alone, significant amounts of IL-2 were detectable in CD4+CD7+ cell supernatants only; conversely, IL-4 and IL-10 could be detected only in the culture medium from CD4+CD7- T cells. This profile of cytokine production was maintained both over time and at the clonal cell level in the CD4+CD7- T cell subset. In HIV-infected patients, the CD4+CD7- T cell expansion observed in relationship with disease progression was associated to an in vivo activation of the CD4+CD7- cells, as assessed by cell surface expression of the HLA-DR, CD25, CD71, and CD57 markers. The CD4+CD7- T cells from HIV-seropositive patients showed the same imbalance of cell proliferation and IL-2, IL-4, and IL-10 production as observed in normal donors despite low levels of proliferation and cytokine production. Together, our data indicate that the lack of CD7 expression defines a CD4+ Th cell subset with a Th0/Th2-like profile of cytokine secretion in normal individuals. The CD4+CD7- subset is expanded during HIV infection and characterized by the same although impaired profile of cytokine production. These CD4+CD7- T cells might play a role in the Th cell dysfunctions observed in HIV infection.

摘要

我们之前报道过,在HIV感染期间,有一部分CD4+ T细胞会扩增,其特征是缺乏CD7细胞表面表达。与正常供体中的CD4+CD7+ 自体细胞相比,这个CD4+CD7- 亚群在CD3触发或CD28共刺激后细胞增殖较低。我们的目的是进一步表征这个CD4+CD7- T细胞亚群在正常供体和HIV感染患者中的Th功能。在对CD3和CD28途径进行细胞分选和共刺激后,分析了它们的CD4+CD7- 细胞增殖和细胞因子分泌情况。在正常供体中,CD4+CD7- 细胞在CD3加CD28共刺激下产生的IL-2占自体CD4+CD7+ 细胞IL-2分泌量的50±28%。此外,CD4+CD7- T细胞产生的IL-4和IL-10量高于CD4+CD7+ 细胞,IL-4和IL-10的平均CD4+CD7-:CD4+CD7+ 比值分别为5.4±4.5和26±25,而两个亚群中IFN-γ的产生相似。仅在单独触发CD3复合物后,仅在CD4+CD7+ 细胞上清液中可检测到大量IL-2;相反,IL-4和IL-10仅在CD4+CD7- T细胞的培养基中可检测到。这种细胞因子产生模式在CD4+CD7- T细胞亚群中随时间推移以及在克隆细胞水平上均得以维持。在HIV感染患者中,与疾病进展相关的CD4+CD7- T细胞扩增与CD4+CD7- 细胞的体内激活有关,这通过HLA-DR、CD25、CD71和CD57标志物的细胞表面表达来评估。尽管HIV血清阳性患者的CD4+CD7- T细胞增殖水平和细胞因子产生水平较低,但与正常供体中观察到的情况一样,其细胞增殖以及IL-2、IL-4和IL-10产生存在相同的失衡。总之,我们的数据表明,CD7表达的缺乏定义了一个在正常个体中具有类似Th0/Th2细胞因子分泌谱的CD4+ Th细胞亚群。CD4+CD7- 亚群在HIV感染期间会扩增,并且具有相同的尽管受损但仍有的细胞因子产生谱。这些CD4+CD7- T细胞可能在HIV感染中观察到的Th细胞功能障碍中起作用。

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