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The transcription of FOXO genes is stimulated by FOXO3 and repressed by growth factors.

机译:FOXO3基因的转录受到FOXO3的刺激,并被生长因子所抑制。

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摘要

Forkhead box O (FOXO) transcription factors induce cell growth arrest and apoptosis, which can be prevented by FOXO phosphorylation by AKT in response to growth factors such as platelet-derived growth factors (PDGF). Beside this well-characterized post-translational modification, we showed that FOXO1, FOXO3 and FOXO4 were also regulated at the transcriptional level. PDGF, FGF and IGF-I repressed the expression of FOXO genes in human fibroblasts. This process was sensitive to phosphatidylinositol-3 kinase inhibition by LY294002. FOXO1-specific shRNA decreased FOXO1 mRNA expression and enhanced fibroblast proliferation, mimicking the effects of growth factors. Conversely, ectopic FOXO3 activation blocked the proliferation of fibroblasts, and induced the expression of FOXO1, FOXO4 and p27-KIP1. Using luciferase reporter assays and chromatin immunoprecipitations, we identified a conserved FOXO-binding site in the promoter of the FOXO1 gene, which was required for regulation by PDGF, and mediated the upregulation of FOXO1 by itself and by FOXO3. Altogether, our results suggest that the expression of FOXO1 and FOXO4 genes is stimulated by FOXO3 and possibly by other FOXO factors in a positive feedback loop, which is disrupted by growth factors.
机译:叉头盒O(FOXO)转录因子诱导细胞生长停滞和凋亡,可通过响应诸如血小板衍生生长因子(PDGF)等生长因子的AKT进行FOXO磷酸化来预防。除了这种特征明确的翻译后修饰外,我们还显示FOXO1,FOXO3和FOXO4在转录水平上也受到调控。 PDGF,FGF和IGF-1抑制人成纤维细胞中FOXO基因的表达。该过程对LY294002对磷脂酰肌醇-3激酶的抑制敏感。 FOXO1特异的shRNA降低FOXO1 mRNA表达并增强成纤维细胞增殖,模仿了生长因子的作用。相反,异位FOXO3激活阻止了成纤维细胞的增殖,并诱导了FOXO1,FOXO4和p27-KIP1的表达。使用萤光素酶报告基因测定和染色质免疫沉淀,我们在FOXO1基因的启动子中鉴定了一个保守的FOXO结合位点,这是PDGF调节所必需的,并介导了FOXO1自身和FOXO3的上调。总之,我们的结果表明,FOXO3和FOXO4可能刺激了正反馈回路中的FOXO1和FOXO4基因的表达,而正反馈回路却被生长因子破坏了。

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