首页> 外文期刊>European Journal of Immunology >CD38 identifies a hypo-proliferative IL-13-secreting CD4+ T-cell subset that does not fit into existing naive and memory phenotype paradigms.
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CD38 identifies a hypo-proliferative IL-13-secreting CD4+ T-cell subset that does not fit into existing naive and memory phenotype paradigms.

机译:CD38识别hypo-proliferative这并不IL-13-secreting CD4 + t细胞子集适应现有的天真和内存表型范例。

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摘要

CD38 is commonly regarded as an activation marker for human T cells. Herein, we show that CD38 expression identifies a hypo-proliferative CD4(+) T-cell subset that, following TCR stimulation, retains expression of naive cell surface markers including CD45RA, CD62L and CCR7. Hypo-proliferation was mediated by reduced CD25 up-regulation upon TCR stimulation compared to CD4(+) CD38(-) cells and lack of responsiveness to exogenous IL-2. Instead, CD4(+) CD38(+) T cells expressed CD127, and hypo-proliferation was reversed by addition of IL-7, further associated with increased STAT5 phosphorylation. This phenotype was exacerbated by addition of an agonistic CD38-binding antibody, suggesting that signaling through CD38 promotes this cell profile. Activated CD4(+) CD38(+) cells had a bias towards IL-13 secretion, but not other Th2 cytokines such as IL-4 or IL-5. In comparison, the CD4(+) CD38(-) cells had a clear bias towards secretion of Th1-associated cytokines IFN-gamma and TNF. The existence of such CD4(+) CD38(+) T cells may play an important role in pathologies such as asthma, which are associated with IL-13, but not IL-4 and IL-5. Coupled with responsiveness to IL-7 but not IL-2, and the involvement of CD38 ligation, our results highlight a unique T-cell subpopulation that does not fit into existing naive and memory cell paradigms.
机译:CD38通常被视为一个激活标记对人类T细胞。表情识别hypo-proliferative CD4 (+)t细胞子集,细胞刺激后,保留天真的细胞表面标记物的表达包括CD45RA、CD62L和CCR7。Hypo-proliferation被减少CD25介导老年病TCR刺激相比CD38 CD4(+)(-)细胞和响应能力的缺乏外生- 2。细胞表达CD127, hypo-proliferation逆转IL-7之外,进一步联系增加STAT5磷酸化。表型是加剧了添加一个织CD38-binding抗体,说明信号通过CD38促进这个细胞概要文件。偏向IL-13分泌,但不是其他Th2细胞因子il - 4或IL-5等。CD38 CD4(+)(-)细胞有明显的偏向IFN-gamma Th1-associated细胞因子的分泌和肿瘤坏死因子。在病态细胞可能起着重要的作用如哮喘与IL-13相关联,但不是il - 4和IL-5。响应IL-7但不2,CD38结扎的参与,我们的结果突出一个独特的t细胞亚群不适合现有的天真和存储单元范例。

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