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Potential targets of FOXL2, a transcription factor involved in craniofacial and follicular development, identified by transcriptomics

机译:FOXL2的潜在靶标,由转录组学鉴定,涉及颅面和卵泡发育的转录因子

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摘要

FOXL2 is a gene encoding a forkhead transcription factor, whose mutations are responsible for the blepharophimosis-ptosis-epicanthus inversus syndrome that often involves premature ovarian failure. FOXL2 is one of the earliest ovarian markers and it offers, along with its targets, an excellent model to study ovarian development and function in normal and pathological conditions. We have recently shown that the aromatase gene is a target of FOXL2, and only three other targets have been reported so far. To detect potential transcriptional targets of FOXL2, we used DNA chips and quantitative PCR to compare the transcriptomes of granulosa-like cells overexpressing, or not, FOXL2. This analysis showed that mediators of inflammation, apoptotic and transcriptional regulators, genes involved in cholesterol metabolism, and genes encoding enzymes and transcription factors involved in reactive oxygen species detoxification were up-regulated. On the other hand, FOXL2 down-regulated the transcription of several genes involved in proteolysis and signal transduction and in transcription regulation. A bioinformatic analysis was conducted to discriminate between potential target promoters activated and repressed by FOXL2. In addition, the promoters of strongly activated genes were enriched in forkhead recognition sites, suggesting that these genes might be direct FOXL2 targets. Altogether, these results provide insight into the activity of FOXL2 and may help in understanding the mechanisms of pathogenesis of FOXL2 mutations if the targets prove to be the same in the ovary.
机译:FOXL2是一个编码叉头转录因子的基因,其突变是导致常发生卵巢早衰的睑缘下垂-上睑下垂-picpichus inversus综合征的原因。 FOXL2是最早的卵巢标志物之一,它与它的靶标一起提供了一个研究正常和病理条件下卵巢发育和功能的出色模型。我们最近显示,芳香酶基因是FOXL2的靶标,到目前为止,仅报道了其他三个靶标。为了检测FOXL2的潜在转录靶标,我们使用了DNA芯片和定量PCR来比较过表达或不过表达FOXL2的颗粒样细胞的转录组。该分析表明,炎症介质,细胞凋亡和转录调节因子,胆固醇代谢相关基因以及参与活性氧解毒的编码酶和转录因子的基因被上调。另一方面,FOXL2下调了蛋白水解和信号转导以及转录调控中涉及的几个基因的转录。进行了生物信息学分析以区分由FOXL2激活和抑制的潜在靶标启动子。此外,强激活基因的启动子在叉头识别位点富集,表明这些基因可能是直接FOXL2靶标。总之,这些结果提供了对FOXL2活性的洞察力,并且如果靶标在卵巢中被证明是相同的,则可能有助于了解FOXL2突变的发病机理。

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