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Identification of an upstream regulatory element reveals a novel requirement for Ind activity in maintaining ind expression

机译:上游调节元件的鉴定揭示了在维持ind表达中对ind活性的新要求

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摘要

A maternally established gradient of nuclear Dorsal protein is the first step in subdivision of the Drosophila neurectoderm into stripes of homeodomain gene expression. Dorsal in combination with the EGF and TGFβ signaling pathways are key regulators of the expression of the genes ventral nervous system defective (vnd), intermediate neuroblasts defective (ind), and muscle segment homeobox (msh) in the developing neurectoderm. These three genes encode homeodomain transcription factors that can repress each other, which ensures adjacent, non-overlapping expression domains. Expression of vnd, ind, and msh is maintained after decline in EGF and TGFβ signaling, but the relevant positive transcriptional regulators have not yet been defined. Here we show that Ind can bind DNA with the same sequence specificity as its murine ortholog Gsh1. We have identified a novel upstream regulatory element at the ind locus containing predicted Ind binding sites, and we show that Ind activity is both necessary and sufficient for reporter gene expression from this element. We conclude that Ind can act as a transcriptional activator, and that positive autoregulation of Ind is a mechanism for persistent ind expression within the developing embryonic nervous system.
机译:由母体建立的核背蛋白梯度是将果蝇神经胚细分成同源域基因表达条纹的第一步。背侧结合EGF和TGFβ信号通路是发育中的神经直肠中腹侧神经系统缺陷(vnd),中间神经母细胞缺陷(ind)和肌肉节同形异位体(msh)基因表达的关键调节因子。这三个基因编码可互相抑制的同源域转录因子,可确保相邻的非重叠表达域。在EGF和TGFβ信号转导下降后,vnd,ind和msh的表达得以维持,但相关的阳性转录调节因子尚未确定。在这里,我们显示Ind可以结合与其鼠同源基因Gsh1相同的序列特异性的DNA。我们已经在包含预测的Ind结合位点的ind基因座上鉴定了一个新的上游调控元件,并且我们显示Ind活性对于从该元件报告基因表达是必要的和充分的。我们得出的结论是,Ind可以充当转录激活因子,而Ind的正向自动调节是在发育中的胚胎神经系统内持续ind表达的机制。

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