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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Differential utilization of Janus kinase-signal transducer activator of transcription signaling pathways in the stimulation of human natural killer cells by IL-2, IL-12, and IFN-alpha.
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Differential utilization of Janus kinase-signal transducer activator of transcription signaling pathways in the stimulation of human natural killer cells by IL-2, IL-12, and IFN-alpha.

机译:在通过IL-2,IL-12和IFN-α刺激人类自然杀伤细胞中,Janus激酶信号转导通路的转录信号通路激活剂的差异利用。

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IL-2-, IL-12-, and IFN-alpha-mediated signaling pathways were analyzed in primary NK cells and in the NK3.3 cell line. Gel mobility shift and immunoprecipitation analyses revealed that in addition to activating STAT3 (signal transducer and activator of transcription-3) and STAT5, IL-2 induced tyrosine and serine phosphorylation of STAT1 alpha, which formed IFN-gamma-activated sequence-binding complexes by itself and with STAT3. Although IL-2 and IFN-alpha activated STAT1 alpha and STAT5, IL-2 predominantly activated STAT5, while IFN-alpha predominantly activated STAT1 alpha. IL-2 induced less STAT1 alpha activation and IFN-alpha induced greater STAT5 activation in NK3.3 cells compared with preactivated primary NK cells. In NK3.3 cells, IL-2 induced comparable formation of c-fos promoter sis-inducible element IFN-gamma-activated sequence-binding complexes containing STAT3 alone with complexes containing STAT3 and STAT1 alpha, while in preactivated primary NK cells, it preferentially induced complexes containing STAT3 and STAT1 alpha. Thus, signaling in NK3.3 cells is not always identical with that in primary NK cells. In contrast to IL-2 and IFN-alpha, IL-12 induced strong tyrosine phosphorylation of STAT4 and variable weak phosphorylation of STAT3. However, supershift analyses using the c-fos promoter sis-inducible element probe showed that IL-12 activated STAT4, STAT1 alpha, and STAT3, and induced complexes containing STAT4 only, STAT4 with STAT1 alpha, STAT3 with STAT1 alpha, or STAT1 alpha only in preactivated primary NK cells. STAT1 alpha activation by IL-12 correlated with increased phosphorylation of serine, but not tyrosine. Finally, IL-2 induced tyrosine phosphorylation of JAK1 and JAK3, while IL-12 induced phosphorylation of JAK2 and TYK2 in both preactivated primary NK and NK3.3 cells. Differential phosphorylation and consequent differential activation of both separate and overlapping STAT proteins by IL-2, IL-12, and IFN-alpha may provide a molecular basis for the similarities and differences in the actions of these cytokines on NK cells.
机译:在原代NK细胞和NK3.3细胞系中分析了IL-2-,IL-12-和IFN-α介导的信号通路。凝胶迁移率变化和免疫沉淀分析表明,除了激活STAT3(信号转导和转录激活因子3)和STAT5外,IL-2还诱导STAT1α的酪氨酸和丝氨酸磷酸化,并通过IFN-γ激活序列结合复合物本身以及STAT3。尽管IL-2和IFN-α激活STAT1 alpha和STAT5,IL-2主要激活STAT5,而IFN-α主要激活STAT1 alpha。与预先活化的原代NK细胞相比,IL-2在NK3.3细胞中诱导的STAT1α活化较少,而IFN-α诱导的STAT5活化较大。在NK3.3细胞中,IL-2诱导仅含STAT3的c-fos启动子诱导诱导因子IFN-γ激活的序列结合复合物与含STAT3和STAT1α的复合物的形成相当,而在预激活的原代NK细胞中,它优先诱导的含有STAT3和STAT1 alpha的复合物。因此,NK3.3细胞中的信号并不总是与原代NK细胞中的信号相同。与IL-2和IFN-α相反,IL-12诱导STAT4的强酪氨酸磷酸化和STAT3的可变弱磷酸化。但是,使用c-fos启动子sis可诱导元件探针进行的超位移分析显示,IL-12激活STAT4,STAT1 alpha和STAT3,并诱导仅包含STAT4,STAT4与STAT1 alpha,STAT3与STAT1 alpha或仅STAT1 alpha的复合物。在预激活的原代NK细胞中。 IL-12对STAT1α的激活与丝氨酸的磷酸化增加有关,但与酪氨酸无关。最后,IL-2诱导JAK1和JAK3的酪氨酸磷酸化,而IL-12诱导了预激活的原代NK和NK3.3细胞的JAK2和TYK2磷酸化。 IL-2,IL-12和IFN-α分别和重叠的STAT蛋白的差异磷酸化以及随后的差异活化可能为这些细胞因子对NK细胞作用的相似性和差异提供分子基础。

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