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小鼠胚胎发育过程中Hoxc-8的调控:早期神经管表达相关关键元件的鉴定与特征分析

Regulation of Hoxc-8 during mouse embryonic development: identification and characterization of critical elements involved in early neural tube expression.

作者信息

Shashikant C S, Bieberich C J, Belting H G, Wang J C, Borbély M A, Ruddle F H

机构信息

Department of Biology, Yale University, New Haven CT 06520, USA.

出版信息

Development. 1995 Dec;121(12):4339-47. doi: 10.1242/dev.121.12.4339.

Abstract

We have characterized cis-acting elements that direct the early phase of Hoxc-8 expression using reporter gene analysis in transgenic mice. By deletion we show that a 135 bp DNA fragment, located approximately 3 kb upstream of the coding region of Hoxc-8, is capable of directing posterior neural tube expression. This early neural tube (ENT) enhancer consists of four separate elements, designated A, B, C and D, whose nucleotide sequences are similar to binding sites of known transcription factors. Nucleotide substitutions suggest that element A is an essential component of the ENT enhancer. However element A by itself is incapable of directing neural tube expression. This element requires interactions at any two of the other three elements, B, C or D. Thus, the components of the ENT enhancer direct neural tube expression in an interdependent manner. We propose that Hoxc-8 is activated in the neural tube by combinatorial interactions among several proteins acting within a small region. Our transgenic analyses provide a means to identify transcription factors that regulate Hoxc-8 expression during embryogenesis.

摘要

我们利用转基因小鼠中的报告基因分析,对指导Hoxc-8表达早期阶段的顺式作用元件进行了表征。通过缺失实验,我们发现位于Hoxc-8编码区上游约3 kb处的一个135 bp DNA片段能够指导神经管后部的表达。这个早期神经管(ENT)增强子由四个独立的元件组成,分别命名为A、B、C和D,其核苷酸序列与已知转录因子的结合位点相似。核苷酸取代表明元件A是ENT增强子的一个重要组成部分。然而,元件A本身无法指导神经管的表达。该元件需要与其他三个元件(B、C或D)中的任意两个相互作用。因此,ENT增强子的各个组成部分以相互依赖的方式指导神经管的表达。我们提出,Hoxc-8在神经管中是通过在一个小区域内起作用的几种蛋白质之间的组合相互作用而被激活的。我们的转基因分析提供了一种方法,用于鉴定在胚胎发育过程中调节Hoxc-8表达的转录因子。

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