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围绕 Hox4 基因的序列保守性的顺式调控特征分析。

Cis-regulatory characterization of sequence conservation surrounding the Hox4 genes.

机构信息

Carl von Ossietzky University, Oldenburg, Germany.

出版信息

Dev Biol. 2010 Apr 15;340(2):269-82. doi: 10.1016/j.ydbio.2010.01.035. Epub 2010 Feb 6.

DOI:10.1016/j.ydbio.2010.01.035
PMID:20144609
Abstract

Hox genes are key regulators of anterior-posterior axis patterning and have a major role in hindbrain development. The zebrafish Hox4 paralogs have strong overlapping activities in hindbrain rhombomeres 7 and 8, in the spinal cord and in the pharyngeal arches. With the aim to predict enhancers that act on the hoxa4a, hoxb4a, hoxc4a and hoxd4a genes, we used sequence conservation around the Hox4 genes to analyze all fish:human conserved non-coding sequences by reporter assays in stable zebrafish transgenesis. Thirty-four elements were functionally tested in GFP reporter gene constructs and more than 100 F1 lines were analyzed to establish a correlation between sequence conservation and cis-regulatory function, constituting a catalog of Hox4 CNEs. Sixteen tissue-specific enhancers could be identified. Multiple alignments of the CNEs revealed paralogous cis-regulatory sequences, however, the CNE sequence similarities were found not to correlate with tissue specificity. To identify ancestral enhancers that direct Hox4 gene activity, genome sequence alignments of mammals, teleosts, horn shark and the cephalochordate amphioxus, which is the most basal extant chordate possessing a single prototypical Hox cluster, were performed. Three elements were identified and two of them exhibited regulatory activity in transgenic zebrafish, however revealing no specificity. Our data show that the approach to identify cis-regulatory sequences by genome sequence alignments and subsequent testing in zebrafish transgenesis can be used to define enhancers within the Hox clusters and that these have significantly diverged in their function during evolution.

摘要

Hox 基因是前后轴模式形成的关键调节因子,在后脑发育中起主要作用。斑马鱼 Hox4 同源物在后脑神经节 7 和 8、脊髓和咽弓中具有强烈的重叠活性。为了预测作用于 hoxa4a、hoxb4a、hoxc4a 和 hoxd4a 基因的增强子,我们使用 Hox4 基因周围的序列保守性通过稳定的斑马鱼转基因报告基因实验来分析所有鱼类:人类保守非编码序列。对 34 个元件进行了 GFP 报告基因构建体的功能测试,分析了 100 多个 F1 系以建立序列保守性和顺式调控功能之间的相关性,构成了 Hox4CNE 目录。可以鉴定出 16 个组织特异性增强子。CNE 的多重比对揭示了旁系同源的顺式调控序列,但是 CNE 序列相似性与组织特异性没有相关性。为了鉴定指导 Hox4 基因活性的祖先增强子,我们对哺乳动物、硬骨鱼、角鲨和头索动物文昌鱼进行了基因组序列比对,文昌鱼是现存最基础的具有单个原型 Hox 簇的脊索动物。鉴定出三个元件,其中两个在转基因斑马鱼中具有调节活性,但没有特异性。我们的数据表明,通过基因组序列比对识别顺式调控序列并随后在斑马鱼转基因中进行测试的方法可用于定义 Hox 簇内的增强子,并且这些增强子在进化过程中其功能已经显著分化。

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