淋巴因子
细胞生物学
离子霉素
细胞毒性T细胞
细胞因子
颗粒酶
生物
胞吐
细胞内
免疫学
免疫系统
穿孔素
分泌物
体外
生物化学
作者
Joy D. Bonnema,Kenneth Rivlin,Adrian T. Ting,Renee A. Schoon,Robert T. Abraham,Paul J. Leibson
出处
期刊:Journal of Immunology
[American Association of Immunologists]
日期:1994-03-01
卷期号:152 (5): 2098-2104
被引量:69
标识
DOI:10.4049/jimmunol.152.5.2098
摘要
NK cells are a subpopulation of lymphocytes that kill virally infected cells and tumor cells without previous sensitization. Although exposure to distinct cytokines, including IL-2 and IL-12, can enhance these cytotoxic responses, the mechanism of this lymphokine-augmented killing remains unclear. Inasmuch as the cytotoxic event is a multistep process, there are many potential targets for lymphokine regulation. We focused on whether selected lymphokines directly modulate the intracellular signaling pathways critical for NK cell secretory function. In our experimental model, homogeneous, cloned human CD16+/CD3- NK cells were pretreated with either IL-2 or IL-12 and then stimulated with direct pharmacologic activators of the secretory response (e.g., PMA and ionomycin for intact cells or GTP gamma S for streptolysin-O permeabilized cells). Previous exposure of the cells to IL-2 or IL-12 enhanced the stimulus-induced release of granule-derived proteins (hexosaminidase and serine proteases) in a cytokine concentration- and time-dependent fashion. Furthermore, the cytokines increased the efficacies without changing the potencies of the secretagogues used in these studies. These results suggest that IL-2 and IL-12 augment NK cell-mediated cytotoxicity by increasing the maximal level of granule exocytosis evoked by Ca2+ and/or G protein-dependent intracellular signaling pathways.
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