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首页> 外文期刊>Gene Regulation and Systems Biology >Identification of cis-Regulatory Elements in the dmyc Gene of Drosophila Melanogaster
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Identification of cis-Regulatory Elements in the dmyc Gene of Drosophila Melanogaster

机译:果蝇dmyc基因顺式调控元件的鉴定。

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Myc is a crucial regulator of growth and proliferation during animal development. Many signals and transcription factors lead to changes in the expression levels of Drosophila myc, yet no clear model exists to explain the complexity of its regulation at the level of transcription. In this study we used Drosophila genetic tools to track the dmyc cis-regulatory elements. Bioinformatics analyses identified conserved sequence blocks in the noncoding regions of the dmyc gene. Investigation of lacZ reporter activity driven by upstream, downstream, and intronic sequences of the dmyc gene in embryonic, larval imaginal discs, larval brain, and adult ovaries, revealed that it is likely to be transcribed from multiple transcription initiation units including a far upstream regulatory region, a TATA box containing proximal complex and a TATA-less downstream promoter element in conjunction with an initiator within the intron 2 region. Our data provide evidence for a modular organization of dmyc regulatory sequences; these modules will most likely be required to generate the tissue-specific patterns of dmyc transcripts. The far upstream region is active in late embryogenesis, while activity of other cis elements is evident during embryogenesis, in specific larval imaginal tissues and during oogenesis. These data provide a framework for further investigation of the transcriptional regulatory mechanisms of dmyc.
机译:Myc是动物发育过程中生长和增殖的关键调节剂。许多信号和转录因子导致果蝇myc表达水平的变化,但尚无明确的模型来解释其在转录水平调控的复杂性。在这项研究中,我们使用果蝇遗传工具来跟踪dmyc顺式调节元件。生物信息学分析了dmyc基因非编码区中已鉴定的保守序列区块。对由dmyc基因的上游,下游和内含子序列驱动的lacZ报告基因活性的研究,该基因位于胚胎,幼虫假想盘,幼虫脑和成年卵巢中,发现它很可能是从多个转录起始单元转录而成的,包括远上游的调控因子区域内,含有近端复合物的TATA盒和无TATA的下游启动子元件与内含子2区域内的引发剂结合。我们的数据为dmyc调控序列的模块化组织提供了证据。这些模块很可能是生成dmyc转录本的组织特异性模式所必需的。远上游区域在晚期胚胎发生中有活性,而其他顺式元件的活性在胚胎发生过程中,特定的幼虫假体组织中和卵子发生过程中很明显。这些数据为进一步研究dmyc的转录调控机制提供了框架。

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