首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Functional consequences of interleukin 2 receptor expression on resting human lymphocytes. Identification of a novel natural killer cell subset with high affinity receptors
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Functional consequences of interleukin 2 receptor expression on resting human lymphocytes. Identification of a novel natural killer cell subset with high affinity receptors

机译:白细胞介素2受体表达对静止的人类淋巴细胞的功能后果。具有高亲和力受体的新型自然杀伤细胞亚群的鉴定

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摘要

In this study, we have used radiolabeled IL-2 binding assays, Northern blot analysis, immunofluorescent flow cytometry and cell sorting, as well as proliferation and cytotoxicity assays to perform an extensive phenotypic and functional characterization of the IL-2 receptor in normal resting human peripheral blood lymphocytes. Our results indicate that almost all T cells (greater than 98%) express neither the high affinity IL-2 receptor nor the functional intermediate affinity p75 chain of the IL-2 receptor without prior activation. In contrast, most NK cells constitutively express the isolated intermediate affinity p75 IL-2 receptor. In addition, a subpopulation of NK cells, distinguished by high density expression of the NKH1 antigen, constitutively express the high affinity IL-2 receptor, in addition to an excess of the isolated intermediate affinity p75 IL-2 receptor. These NKH1bright+ cells exhibit a brisk proliferative response to IL-2, similar to that seen with antigen-activated T cells, yet do so in the absence of any known antigenic stimuli. No other resting peripheral blood lymphocyte population, including CD4+, CD8+, and CD20 cells, exhibits this property. The intermediate affinity p75 IL-2 receptor, as it exists in its isolated form on resting NK cells, does not transduce a growth signal equivalent to that seen in NK cells expressing the high affinity IL-2 receptor, despite doses of IL-2 that are known to fully saturate the isolated p75 chain. This strongly suggests that additional structural or functional components are involved in generating the proliferative response following the binding of IL-2 to the high affinity heterodimeric form of the IL-2 receptor. The constitutive expression of this functional high affinity IL-2 receptor on a small population of resting NK cells provides further evidence in support of a role for these cells in the host's early defense against viral infection or malignant transformation, before the more delayed but specific T cell response.
机译:在这项研究中,我们使用了放射性标记的IL-2结合测定,Northern印迹分析,免疫荧光流式细胞术和细胞分选以及增殖和细胞毒性测定,对正常静止的人进行IL-2受体的广泛表型和功能表征外周血淋巴细胞。我们的结果表明,几乎所有T细胞(大于98%)既不表达高亲和力IL-2受体,也不表达IL-2受体的功能性中间亲和力p75链,而无需事先激活。相反,大多数NK细胞组成性表达分离的中间亲和力p75 IL-2受体。此外,除了过量的分离的中间亲和力p75 IL-2受体外,以NKH1抗原的高密度表达为特征的NK细胞亚群组成性表达高亲和力IL-2受体。这些NKH1bright +细胞表现出对IL-2的快速增殖反应,与抗原激活的T细胞相似,但是在没有任何已知抗原刺激的情况下却如此。没有其他静止的外周血淋巴细胞群体,包括CD4 +,CD8 +和CD20细胞,表现出这种特性。中间亲和力p75 IL-2受体(以分离形式存在于静止的NK细胞上)不传递与表达高亲和力IL-2受体的NK细胞相同的生长信号,尽管剂量的IL-2已知完全饱和分离的p75链。这强烈暗示在IL-2与IL-2受体的高亲和力异二聚体形式结合后,在产生增殖应答中涉及其他结构或功能组分。这种功能性高亲和力IL-2受体在少量静止的NK细胞上的组成型表达提供了进一步的证据,支持这些细胞在宿主延迟防御特异性T之前对病毒感染或恶性转化的早期防御中的作用。细胞反应。

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