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果蝇胚胎中无翅基因的表达:patched介导的抑制作用需要一个缺乏保守Ci结合位点的保守顺式作用元件。

Expression of wingless in the Drosophila embryo: a conserved cis-acting element lacking conserved Ci-binding sites is required for patched-mediated repression.

作者信息

Lessing D, Nusse R

机构信息

Howard Hughes Medical Institute, Department of Developmental Biology, Beckman Center, Stanford University, Medical Center, Stanford, CA 94305, USA.

出版信息

Development. 1998 Apr;125(8):1469-76. doi: 10.1242/dev.125.8.1469.

Abstract

Patterning of the Drosophila embryo depends on the accurate expression of wingless (wg), which encodes a secreted signal required for segmentation and many other processes. Early expression of wg is regulated by the nuclear proteins of the gap and pair-rule gene classes but, after gastrulation, wg transcription is also dependent on cell-cell communication. Signaling to the Wg-producing cells is mediated by the secreted protein, Hedgehog (Hh), and by Cubitus interruptus (Ci), a transcriptional effector of the Hh signal transduction pathway. The transmembrane protein Patched (Ptc) acts as a negative regulator of wg expression; ptc- embryos have ectopic wg expression. According to the current models, Ptc is a receptor for Hh. The default activity of Ptc is to inhibit Ci function; when Ptc binds Hh, this inhibition is released and Ci can control wg transcription. We have investigated cis-acting sequences that regulate wg during the time that wg expression depends on Hh signaling. We show that approximately 4.5 kb immediately upstream of the wg transcription unit can direct expression of the reporter gene lacZ in domains similar to the normal wg pattern in the embryonic ectoderm. Expression of this reporter construct expands in ptc mutants and responds to hh activity. Within this 4.5 kb, a 150 bp element, highly conserved between D. melanogaster and Drosophila virilis, is required to spatially restrict wg transcription. Activity of this element depends on ptc, but it contains no consensus Ci-binding sites. The discovery of an element that is likely to bind a transcriptional repressor was unexpected, since the prevailing model suggests that wg expression is principally controlled by Hh signaling acting through the Ci activator. We show that wg regulatory DNA can drive lacZ in a proper wg-like pattern without any conserved Ci-binding sites and suggest that Ci can not be the sole endpoint of the Hh pathway.

摘要

果蝇胚胎的模式形成依赖于无翅基因(wg)的精确表达,该基因编码一种参与体节形成及许多其他过程所需的分泌信号。wg的早期表达受间隙基因和成对规则基因类别的核蛋白调控,但在原肠胚形成后,wg转录也依赖于细胞间通讯。向产生Wg的细胞发出信号是由分泌蛋白刺猬蛋白(Hh)以及Hh信号转导途径的转录效应因子间断翅脉蛋白(Ci)介导的。跨膜蛋白patched(Ptc)作为wg表达的负调控因子;ptc突变体胚胎具有异位wg表达。根据当前模型,Ptc是Hh的受体。Ptc的默认活性是抑制Ci功能;当Ptc结合Hh时,这种抑制作用被解除,Ci可以控制wg转录。我们研究了在wg表达依赖于Hh信号传导期间调控wg的顺式作用序列。我们发现,wg转录单元上游约4.5 kb的区域可在胚胎外胚层中指导报告基因lacZ在与正常wg模式相似的区域表达。该报告构建体的表达在ptc突变体中扩展,并对hh活性作出反应。在这4.5 kb区域内,一个150 bp的元件在黑腹果蝇和果蝇属之间高度保守,它对于在空间上限制wg转录是必需的。该元件的活性依赖于ptc,但它不包含共有Ci结合位点。发现一个可能结合转录抑制因子的元件是出乎意料的,因为流行的模型表明wg表达主要由通过Ci激活剂起作用的Hh信号传导控制。我们表明wg调控DNA可以在没有任何保守Ci结合位点的情况下以适当的wg样模式驱动lacZ表达,并表明Ci不可能是Hh途径的唯一终点。

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