首页> 美国卫生研究院文献>PLoS Genetics >The bHLH Factors Extramacrochaetae and Daughterless Control Cell Cycle in Drosophila Imaginal Discs through the Transcriptional Regulation of the cdc25 Phosphatase string
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The bHLH Factors Extramacrochaetae and Daughterless Control Cell Cycle in Drosophila Imaginal Discs through the Transcriptional Regulation of the cdc25 Phosphatase string

机译:bHLH因子果蝇假想盘中的宏观调控和无子代控制细胞周期通过转录调控的cdc25磷酸酶串。

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摘要

One of the major issues in developmental biology is about having a better understanding of the mechanisms that regulate organ growth. Identifying these mechanisms is essential to understand the development processes that occur both in physiological and pathological conditions, such as cancer. The E protein family of basic helix-loop helix (bHLH) transcription factors, and their inhibitors the Id proteins, regulate cell proliferation in metazoans. This notion is further supported because the activity of these factors is frequently deregulated in cancerous cells. The E protein orthologue Daughterless (Da) and the Id orthologue Extramacrochaetae (Emc) are the only members of these classes of bHLH proteins in Drosophila. Although these factors are involved in controlling proliferation, the mechanism underlying this regulatory activity is poorly understood. Through a genetic analysis, we show that during the development of epithelial cells in the imaginal discs, the G2/M transition, and hence cell proliferation, is controlled by Emc via Da. In eukaryotic cells, the main activator of this transition is the Cdc25 phosphatase, string. Our genetic analyses reveal that the ectopic expression of string in cells with reduced levels of Emc or high levels of Da is sufficient to rescue the proliferative defects seen in these mutant cells. Moreover, we present evidence demonstrating a role of Da as a transcriptional repressor of string. Taken together, these findings define a mechanism through which Emc controls cell proliferation by regulating the activity of Da, which transcriptionally represses string.
机译:发育生物学的主要问题之一是要更好地了解调节器官生长的机制。识别这些机制对于理解发生在生理和病理状况(例如癌症)中的发育过程至关重要。碱性螺旋环螺旋(bHLH)转录因子的E蛋白家族及其抑制剂Id蛋白调节后生动物中的细胞增殖。由于癌细胞中这些因子的活性经常被失调,因此这一观点得到了进一步的支持。 E蛋白直系同源的无子代(Da)和Id直系同源的超外生菌(Emc)是果蝇中这类bHLH蛋白的唯一成员。尽管这些因素参与了控制增殖,但对这种调节活性的机制却知之甚少。通过遗传分析,我们显示,在视盘中上皮细胞的发育过程中,Emc通过Da控制G2 / M过渡以及细胞增殖。在真核细胞中,这种转变的主要激活因子是Cdc25磷酸酶,即字符串。我们的遗传分析表明,在Emc含量降低或Da含量高的细胞中,字符串的异位表达足以挽救在这些突变细胞中看到的增殖缺陷。此外,我们目前的证据表明Da作为字符串的转录阻遏物。综上所述,这些发现确定了Emc通过调节Da的活性来控制细胞增殖的机制,Da的转录可抑制弦乐。

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