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E2F-1 regulates expression of FOXO1 and FOXO3a

机译:E2F-1调节FOXO1和FOXO3a的表达

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E2F and FOXO transcription factors both play a role in neuronal apoptosis. In addition, both E2F-induced apoptosis and FOXO function are inhibited by the kinase Akt. We therefore tested whether FOXO is downstream of E2F-1 during neuronal apoptosis. We found that expression of endogenous FOXO1 and FOXO3 alpha is induced by E2F-1. The presence of putative E2F binding sites in the promoters of both genes suggested that FOXO genes are direct targets of E217-1. Indeed, a4-hydroxytamoxifen activated E2F-1-ER fusion protein induced FOXO expression in the presence of cycloheximide. Moreover, E2F-1 activated the FOXO1 promoter in transient reporter assays, and E2F-1-ER as well as endogenous E2F bound to the FOXO1 promoter in vivo. Yet, E2F-1-mediated apoptosis of differentiated PC12 cells after withdrawal of NGF was not accompanied by changes in FOXO expression, indicating that no transcriptional induction of FOXO occurs during E2F-1-dependent neuronal apoptosis. In summary, our data identify E2F-1 as a first transcription factor regulating FOXO expression, providing a link between E2F and FOXO proteins in the control of cell fate. (C) 2007 Elsevier B.V. All rights reserved.
机译:E2F和FOXO转录因子均在神经元凋亡中起作用。另外,E2F诱导的细胞凋亡和FOXO功能均被激酶Akt抑制。因此,我们测试了神经元凋亡过程中FOXO是否在E2F-1的下游。我们发现内源性FOXO1和FOXO3 alpha的表达是由E2F-1诱导的。两个基因的启动子中均存在推定的E2F结合位点,这表明FOXO基因是E217-1的直接靶标。实际上,在存在环己酰亚胺的情况下,α4-羟基他莫昔芬激活的E2F-1-ER融合蛋白诱导了FOXO表达。此外,E2F-1在瞬时报告基因检测中激活了FOXO1启动子,并且E2F-1-ER以及内源性E2F在体内均与FOXO1启动子结合。然而,NGF撤离后,E2F-1介导的分化PC12细胞的凋亡并未伴随FOXO表达的变化,这表明在E2F-1依赖性神经元凋亡期间未发生FOXO的转录诱导。总而言之,我们的数据确定E2F-1是调节FOXO表达的第一个转录因子,在细胞命运控制中提供了E2F和FOXO蛋白之间的联系。 (C)2007 Elsevier B.V.保留所有权利。

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