Narimatsu M, Maeda H, Itoh S, Atsumi T, Ohtani T, Nishida K, Itoh M, Kamimura D, Park S J, Mizuno K, Miyazaki J, Hibi M, Ishihara K, Nakajima K, Hirano T
Department of Molecular Oncology, Osaka University Graduate School of Medicine, Suita, Osaka 565-0871, Japan.
Mol Cell Biol. 2001 Oct;21(19):6615-25. doi: 10.1128/MCB.21.19.6615-6625.2001.
Signal transducer and activator of transcription 3 (STAT3) mediates signals of various growth factors and cytokines, including interleukin-6 (IL-6). In certain IL-6-responsive cell lines, the stat3 gene is autoregulated by STAT3 through a composite IL-6 response element in its promoter that contains a STAT3-binding element (SBE) and a cyclic AMP-responsive element. To reveal the nature and roles of the stat3 autoregulation in vivo, we generated mice that harbor a mutation in the SBE (stat3(mSBE)). The intact SBE was crucial for IL-6-induced stat3 gene activation in the spleen, especially in the red pulp region, the kidney, and both mature and immature T lymphocytes. The SBE was not required, however, for IL-6-induced stat3 gene activation in hepatocytes. T lymphocytes from the stat3(mSBE/mSBE) mice were more susceptible to apoptosis despite the presence of IL-6 than those from wild-type mice. Consistent with this, IL-6-dependent activation of the Pim-1 and junB genes, direct target genes for STAT3, was attenuated in T lymphocytes of the stat3(mSBE/mSBE) mice. Thus, the tissue-specific autoregulation of the stat3 gene operates in vivo and plays a role in IL-6-induced antiapoptotic signaling in T cells.
信号转导及转录激活因子3(STAT3)介导多种生长因子和细胞因子的信号,包括白细胞介素-6(IL-6)。在某些IL-6应答细胞系中,stat3基因通过其启动子中的复合IL-6应答元件由STAT3进行自身调节,该元件包含一个STAT3结合元件(SBE)和一个环磷酸腺苷应答元件。为了揭示体内stat3自身调节的本质和作用,我们构建了在SBE处有突变的小鼠(stat3(mSBE))。完整的SBE对于IL-6诱导的脾脏中stat3基因激活至关重要,尤其是在红髓区域、肾脏以及成熟和未成熟T淋巴细胞中。然而,SBE对于IL-6诱导的肝细胞中stat3基因激活并非必需。尽管存在IL-6,但来自stat3(mSBE/mSBE)小鼠的T淋巴细胞比来自野生型小鼠的T淋巴细胞更容易发生凋亡。与此一致的是,在stat3(mSBE/mSBE)小鼠的T淋巴细胞中,STAT3的直接靶基因Pim-1和junB基因的IL-6依赖性激活减弱。因此,stat3基因的组织特异性自身调节在体内发挥作用,并在IL-6诱导的T细胞抗凋亡信号传导中起作用。
