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通过Fc-γ受体介导的人自然杀伤细胞上活化抗原的诱导。

Induction of activation antigens on human natural killer cells mediated through the Fc-gamma receptor.

作者信息

Harris D T, Travis W W, Koren H S

机构信息

Center for Environmental Medicine and Lung Biology, University of North Carolina, Chapel Hill 27599.

出版信息

J Immunol. 1989 Oct 1;143(7):2401-6.

PMID:2528593
Abstract

NK cells, defined here as lymphocytes bearing the CD16 Ag found on the NK cell Fc-gamma receptor (FcR), are known to enter a proliferative and activated state in response to stimulation with IL-2 as assessed by clonal expansion, short-term DNA synthesis, and de novo expression of lymphocyte-associated activation Ag. We have found that the FcR of NK cells acts as a signaling pathway through which IL-2-dependent activation may be greatly enhanced, allowing for more rapid induction of activation Ag and recruitment of an increased percentage of cells expressing surface markers of cellular activation. FcR-interactive agents, such as solid phase immobilized immune complexes or cross-linked CD16-specific mAb, work synergistically with rIL-2 to elicit a rapid expression of IL2R and transferrin receptors on greater than 50% of purified NK cells as early as day 3 of culture. IL-2 or FcR-interactive stimuli alone were weak or ineffective stimulators by comparison. In contrast to the induction of de novo activation Ag, DNA synthesis was elicited by IL-2 alone, but was not substantially or consistently enhanced by the subsequent addition of FcR-interactive stimuli.

摘要

自然杀伤(NK)细胞,在此定义为带有在NK细胞Fc-γ受体(FcR)上发现的CD16抗原的淋巴细胞,已知其在受到白细胞介素-2(IL-2)刺激后会进入增殖和激活状态,这可通过克隆扩增、短期DNA合成以及淋巴细胞相关激活抗原的从头表达来评估。我们发现,NK细胞的FcR充当一种信号通路,通过该通路,IL-2依赖性激活可能会大大增强,从而能够更快速地诱导激活抗原,并募集更高比例表达细胞激活表面标志物的细胞。FcR相互作用剂,如固相固定的免疫复合物或交联的CD16特异性单克隆抗体,与重组IL-2协同作用,早在培养第3天就能在超过50%的纯化NK细胞上快速诱导IL2R和转铁蛋白受体的表达。相比之下,单独的IL-2或FcR相互作用刺激是较弱或无效的刺激物。与从头诱导激活抗原不同,DNA合成仅由IL-2引发,但随后添加FcR相互作用刺激并不能实质性或持续增强DNA合成。

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