Yu C R, Young H A, Ortaldo J R
Division of Basic Sciences, National Cancer Institute, Frederick Cancer Research and Development Center, National Institutes of Health, Frederick, Maryland 21702-1201, USA.
J Leukoc Biol. 1998 Aug;64(2):245-58. doi: 10.1002/jlb.64.2.245.
Cytokines, IL-2, IL-4, IL-6, IL-7, IL-12, and IL-15 are key regulators of human peripheral blood T and NK cell activation and differentiation but the precise mechanisms that give rise to their differential activities within these cells are not clear. Recent studies reveal that a family of transcription factors, signal transducers and activators of transcription (STATs) directly mediate many cytokine signals. We analyzed the activation of STATs in primary human T and NK cells by a variety of specific cytokines. We demonstrate that IL-12 induces STAT4 only in freshly isolated primary NK cells, but not in primary T cells, consistent with the lack of the IL-12 receptor in resting T cells. In contrast, IL-4 induces different C epsilon GAS DNA-protein binding complexes in both T and NK cells. Moreover, IL-4 costimulation with IL-2 or IL-12 does not alter their own preferential GAS-like DNA binding patterns when C epsilon-, Fc gamma RI-, and SIE GAS motif containing oligonucleotide probes are compared, suggesting that induction of GAS-like DNA-protein binding complexes by IL-2, IL-4, and IL-12 is highly selective and represents one important factor in determining specific gene activation. In addition, IL-6 and IL-2 synergistically induce homo- and heterodimerized STAT1 alpha and STAT3 in both NK and T cells, consistent with their reported synergism in modulating perforin gene expression. We further demonstrated that IL-2, -7, and -15 induce multiple STAT proteins, including STAT5a, STAT5b, STAT1 alpha, STAT3, and another unidentified Fc gamma RI GAS DNA-binding protein. Finally, we observed that activated STAT5a and STAT5b proteins form distinct Fc gamma RI GAS binding patterns in T and NK cells, suggesting that they might have different roles in gene regulation. Our data provide evidence that the differential responses in gene expression and cell activation seen in primary NK and T cells on direct stimulation with different cytokines may be a direct result of distinct activation of STAT transcription factors.
细胞因子白细胞介素-2(IL-2)、白细胞介素-4(IL-4)、白细胞介素-6(IL-6)、白细胞介素-7(IL-7)、白细胞介素-12(IL-12)和白细胞介素-15(IL-15)是人类外周血T细胞和自然杀伤(NK)细胞活化及分化的关键调节因子,但这些细胞内导致它们产生不同活性的精确机制尚不清楚。最近的研究表明,一类转录因子,即信号转导子和转录激活子(STATs)直接介导许多细胞因子信号。我们通过多种特异性细胞因子分析原代人T细胞和NK细胞中STATs的激活情况。我们证明,IL-12仅在新鲜分离的原代NK细胞中诱导STAT4,而不在原代T细胞中诱导,这与静息T细胞中缺乏IL-12受体一致。相反,IL-4在T细胞和NK细胞中诱导不同的CεGAS DNA-蛋白质结合复合物。此外,当比较含有Cε、FcγRI和SIE GAS基序的寡核苷酸探针时,IL-4与IL-2或IL-12共刺激不会改变它们自身偏好的GAS样DNA结合模式,这表明IL-2、IL-4和IL-12对GAS样DNA-蛋白质结合复合物的诱导具有高度选择性,并且是决定特定基因激活的一个重要因素。此外,IL-6和IL-2在NK细胞和T细胞中协同诱导同源和异源二聚化的STAT1α和STAT3,这与它们在调节穿孔素基因表达方面报道的协同作用一致。我们进一步证明,IL-2、IL-7和IL-15诱导多种STAT蛋白,包括STAT5a、STAT5b、STAT1α、STAT3和另一种未鉴定的FcγRI GAS DNA结合蛋白。最后,我们观察到活化的STAT5a和STAT5b蛋白在T细胞和NK细胞中形成不同的FcγRI GAS结合模式,这表明它们在基因调控中可能具有不同的作用。我们的数据提供了证据,即原代NK细胞和T细胞在受到不同细胞因子直接刺激时,在基因表达和细胞活化方面的差异反应可能是STAT转录因子不同激活的直接结果。
