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成纤维细胞生长因子信号传导利用多种机制抑制成骨细胞中Wnt诱导的转录。

Fibroblast growth factor signaling uses multiple mechanisms to inhibit Wnt-induced transcription in osteoblasts.

作者信息

Ambrosetti Davide, Holmes Greg, Mansukhani Alka, Basilico Claudio

机构信息

Department of Microbiology, New York University School of Medicine, New York, NY 10016, USA.

出版信息

Mol Cell Biol. 2008 Aug;28(15):4759-71. doi: 10.1128/MCB.01849-07. Epub 2008 May 27.

Abstract

Fibroblast growth factor (FGF) and Wnt signals are both critical for proper bone development. We previously reported that the expression of activating FGF receptor mutations in osteoblasts downregulated the expression of many genes reported as targets of Wnt signaling, suggesting an antagonistic effect between Wnt signaling, which promotes osteoblast differentiation and function, and FGF signaling, which inhibits these processes. To analyze the effect of FGF on Wnt signaling in osteoblasts, we created reporter cell lines where a Wnt-responsive promoter drives luciferase expression and showed that Wnt3a-induced luciferase expression was specifically inhibited by FGF treatment. FGF specifically prevented the formation of a Wnt-induced transcriptional complex of TCF1 and -4 with beta-catenin on DNA. FGF did not significantly affect the activation of beta-catenin, although it reduced both the expression of TCF/LEF factors and their induction by Wnt. Microarray analysis using osteoblasts treated with Wnt3a and FGF alone or in combination showed that about 70% of the genes induced by Wnt3a were downregulated by combined FGF treatment. These included novel and previously identified Wnt target genes and genes involved in osteoblast differentiation. Furthermore, FGF alone could downregulate the expression of four Fzd Wnt receptor genes. Our results show that FGF antagonizes Wnt signaling by inhibiting Wnt-induced transcription and suggest that multiple mechanisms, including downregulation of TCFs and Wnt receptors, contribute to this effect.

摘要

成纤维细胞生长因子(FGF)和Wnt信号对于正常的骨骼发育均至关重要。我们之前报道过,成骨细胞中激活型FGF受体突变的表达下调了许多被报道为Wnt信号靶点的基因的表达,这表明促进成骨细胞分化和功能的Wnt信号与抑制这些过程的FGF信号之间存在拮抗作用。为了分析FGF对成骨细胞中Wnt信号的影响,我们构建了报告细胞系,其中Wnt反应性启动子驱动荧光素酶表达,并表明FGF处理可特异性抑制Wnt3a诱导的荧光素酶表达。FGF特异性地阻止了TCF1和-4与β-连环蛋白在DNA上形成Wnt诱导的转录复合物。FGF虽然降低了TCF/LEF因子的表达及其被Wnt诱导的水平,但对β-连环蛋白的激活没有显著影响。使用单独或联合Wnt3a和FGF处理的成骨细胞进行的微阵列分析表明,Wnt3a诱导的约70%的基因在联合FGF处理后被下调。这些基因包括新的和先前鉴定的Wnt靶基因以及参与成骨细胞分化的基因。此外,单独的FGF就能下调四种Fzd Wnt受体基因的表达。我们的结果表明,FGF通过抑制Wnt诱导的转录来拮抗Wnt信号,并提示包括TCF和Wnt受体下调在内的多种机制促成了这一效应。

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