成纤维细胞生长因子抑制软骨细胞中的干扰素γ-信号转导和转录激活因子1以及白细胞介素6-信号转导和转录激活因子3信号通路。
Fibroblast growth factor inhibits interferon gamma-STAT1 and interleukin 6-STAT3 signaling in chondrocytes.
作者信息
Krejci Pavel, Prochazkova Jirina, Bryja Vitezslav, Jelinkova Petra, Pejchalova Katerina, Kozubik Alois, Thompson Leslie Michels, Wilcox William R
机构信息
Institute of Experimental Biology, Masaryk University, 61137 Brno, Czech Republic.
出版信息
Cell Signal. 2009 Jan;21(1):151-60. doi: 10.1016/j.cellsig.2008.10.006. Epub 2008 Oct 12.
Abstract
Activation of fibroblast growth factor receptor 3 (FGFR3) leads to attenuation of cartilage growth. The members of the STAT family of transcription factors are believed to participate in FGFR3 signaling in cartilage, however the molecular mechanism of this action is poorly understood. Here, we demonstrate that a chronic FGF stimulus leads to accumulation of STAT1, 3, 5 and 6, evident in both in vitro chondrocyte model and murine limb explant cultures. Despite the accumulation, both endogenous and cytokine-induced activation of STAT1 and STAT3 is impaired by FGF, as demonstrated by imaging of active STAT nuclear translocation and analyses of STAT activatory phosphorylation and transcriptional activation. Further, we demonstrate that FGF induces expression of CIS, SOCS1 and SOCS3 inhibitors of gp130, a common receptor for the IL6-family of cytokines. Since cytokine-gp130 signaling represents an important positive regulator of cartilage, its inhibition may contribute to the growth-inhibitory effect of FGFR3 in cartilage.
摘要
成纤维细胞生长因子受体3(FGFR3)的激活会导致软骨生长减弱。转录因子STAT家族成员被认为参与软骨中的FGFR3信号传导,然而这种作用的分子机制尚不清楚。在此,我们证明慢性FGF刺激会导致STAT1、3、5和6的积累,这在体外软骨细胞模型和小鼠肢体外植体培养中均很明显。尽管有积累,但FGF会损害内源性和细胞因子诱导的STAT1和STAT3激活,这通过活性STAT核转位成像以及STAT激活磷酸化和转录激活分析得以证明。此外,我们证明FGF会诱导CIS、SOCS1和SOCS3的表达,它们是gp130的抑制剂,gp130是IL6细胞因子家族的共同受体。由于细胞因子-gp130信号传导是软骨的重要正调节因子,其抑制可能有助于FGFR3对软骨的生长抑制作用。
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SOCS proteins, cytokine signalling and immune regulation.细胞因子信号抑制蛋白、细胞因子信号传导与免疫调节
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