首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Interleukin 7 enhances cytolytic T lymphocyte generation and induces lymphokine-activated killer cells from human peripheral blood
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Interleukin 7 enhances cytolytic T lymphocyte generation and induces lymphokine-activated killer cells from human peripheral blood

机译:白介素7增强细胞溶解性T淋巴细胞的生成并诱导人外周血中淋巴因子激活的杀伤细胞

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摘要

The effects of purified recombinant interleukin 7 (IL-7) on the generation of cytolytic T lymphocytes (CTL) in mixed lymphocyte culture (MLC) and on the induction of lymphokine-activated killer (LAK) cells in autologous cultures of human peripheral blood mononuclear cells were investigated. IL-7 was found to induce the generation of both CTL and LAK cells in bulk cultures. The appearance of peak CTL activity in MLC established with exogenous IL-7 was delayed in comparison with replicate cultures containing exogenous IL-2, but both cytokines stimulated quantitatively similar levels of antigen-specific lytic activity. An IL-2-neutralizing antiserum inhibited substantially, but not completely, the effect of IL-7 on CTL generation, implying the existence of both an indirect component of IL-7 activity via IL-2 utilization, as well as an IL-2-independent component. Cell surface phenotypic analysis of IL-2- or IL-7-generated CTL effector cells revealed that CD8+ cells were responsible for the vast majority of lytic activity. Limiting dilution analysis (LDA) revealed that essentially identical frequencies of CTL precursors (CTL-P) were capable of clonal expansion and/or differentiation in the presence of exogenous IL-2, IL-4, or IL-7, supporting the concept that all three of these cytokines are capable of exerting a major influence on T cell growth and differentiation. Approximately half of the CTL-P that responded in IL-7-supplemented LDA cultures did so in an IL-2- independent manner. IL-7 stimulated the development of LAK cells in autologous bulk cultures, but only weakly in comparison with IL-2. In contrast to its effects on CTL generation, the induction of LAK cells by IL-7 was virtually independent of IL-2. LAK cells induced by IL-7, like those induced by IL-2, were phenotypically heterogeneous and included CD8+, CD56+, and gamma/delta+ cells. Limiting dilution analysis indicated that IL-2 stimulated fivefold more LAK-P than IL-7 and 220-fold more than IL-4. Collectively, these data suggest that IL-7 has potent regulatory effects on human cytolytic cell populations and, either alone or in combination with other cytokines, could be important for the in vitro expansion of cells for adoptive immunotherapy.
机译:纯化的重组白介素7(IL-7)对混合淋巴细胞培养(MLC)中溶细胞性T淋巴细胞(CTL)的产生以及对人外周血单核自体培养物中淋巴因子激活的杀伤细胞(LAK)的诱导的影响细胞进行了调查。发现IL-7在批量培养中诱导CTL和LAK细胞的产生。与含有外源IL-2的复制培养物相比,用外源IL-7建立的MLC中CTL活性峰值的出现被延迟了,但是两种细胞因子都在数量上刺激了相似水平的抗原特异性裂解活性。 IL-2中和性抗血清基本上(但不完全)抑制IL-7对CTL生成的影响,这暗示着通过IL-2的利用,IL-7活性的间接成分以及IL-2的存在-独立组件。 IL-2或IL-7生成的CTL效应细胞的细胞表面表型分析表明,CD8 +细胞是绝大多数裂解活性的原因。极限稀释分析(LDA)显示,在存在外源IL-2,IL-4或IL-7的情况下,频率基本相同的CTL前体(CTL-P)能够克隆扩增和/或分化,从而支持以下观点:这三种细胞因子均能够对T细胞的生长和分化产生重大影响。在补充了IL-7的LDA培养物中,约有一半的CTL-P以IL-2无关的方式应答。 IL-7刺激了自体大量培养物中LAK细胞的发育,但与IL-2相比只是微弱的。与它对CTL产生的影响相反,IL-7对LAK细胞的诱导实际上独立于IL-2。 IL-7诱导的LAK细胞与IL-2诱导的LAK细胞在表型上异质,包括CD8 +,CD56 +和γ/δ+细胞。极限稀释分析表明,IL-2刺激的LAK-P比IL-7多五倍,比IL-4多220倍。总体而言,这些数据表明,IL-7对人溶细胞细胞群具有有效的调节作用,无论是单独使用还是与其他细胞因子组合使用,IL-7对于过继免疫疗法的细胞体外扩增可能都是重要的。

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