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Dlx5/Dlx6基因间区域中一个高度保守的增强子是胚胎前脑Dlx基因之间交叉调控相互作用的位点。

A highly conserved enhancer in the Dlx5/Dlx6 intergenic region is the site of cross-regulatory interactions between Dlx genes in the embryonic forebrain.

作者信息

Zerucha T, Stühmer T, Hatch G, Park B K, Long Q, Yu G, Gambarotta A, Schultz J R, Rubenstein J L, Ekker M

机构信息

Loeb Health Research Institute at the Ottawa Hospital and Department of Medicine, University of Ottawa, Ottawa, Ontario K1Y 4E9, Canada.

出版信息

J Neurosci. 2000 Jan 15;20(2):709-21. doi: 10.1523/JNEUROSCI.20-02-00709.2000.

Abstract

Four Dlx homeobox genes, Dlx1, Dlx2, Dlx5, and Dlx6 are expressed in the same primordia of the mouse forebrain with temporally overlapping patterns. The four genes are organized as two tail-to-tail pairs, Dlx1/Dlx2 and Dlx5/Dlx6, a genomic arrangement conserved in distantly related vertebrates like zebrafish. The Dlx5/Dlx6 intergenic region contains two sequences of a few hundred base pairs, remarkably well conserved between mouse and zebrafish. Reporter transgenes containing these two sequences are expressed in the forebrain of transgenic mice and zebrafish with patterns highly similar to endogenous Dlx5 and Dlx6 expression. The activity of the transgene is drastically reduced in mouse mutants lacking both Dlx1 and Dlx2, consistent with the decrease in endogenous Dlx5 and Dlx6 expression. These results suggest that cross-regulation by Dlx proteins, mediated by the intergenic sequences, is essential for Dlx5 and Dlx6 expression in the forebrain. This hypothesis is supported by cotransfection and DNA-protein binding experiments. We propose that the Dlx genes are part of a highly conserved developmental pathway that regulates forebrain development.

摘要

四个Dlx同源框基因,即Dlx1、Dlx2、Dlx5和Dlx6,在小鼠前脑的相同原基中表达,且表达模式在时间上有重叠。这四个基因以两个尾对尾的基因对形式排列,即Dlx1/Dlx2和Dlx5/Dlx6,这种基因组排列在斑马鱼等远缘脊椎动物中是保守的。Dlx5/Dlx6基因间区域包含两个几百个碱基对的序列,在小鼠和斑马鱼之间显著保守。含有这两个序列的报告转基因在转基因小鼠和斑马鱼的前脑中表达,其模式与内源性Dlx5和Dlx6的表达高度相似。在同时缺失Dlx1和Dlx2的小鼠突变体中,转基因的活性大幅降低,这与内源性Dlx5和Dlx6表达的减少一致。这些结果表明,由基因间序列介导的Dlx蛋白的交叉调节对于前脑中Dlx5和Dlx6的表达至关重要。这一假设得到了共转染和DNA-蛋白质结合实验的支持。我们提出,Dlx基因是调节前脑发育的高度保守的发育途径的一部分。

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