首页> 外文期刊>Nucleic Acids Research >An ultraconserved Hox-Pbx responsive element resides in the coding sequence of Hoxa2 and is active in rhombomere 4.
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An ultraconserved Hox-Pbx responsive element resides in the coding sequence of Hoxa2 and is active in rhombomere 4.

机译:超保守的Hox-Pbx响应元件位于Hoxa2的编码序列中,并在rhombomere 4中有活性。

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摘要

The Hoxa2 gene has a fundamental role in vertebrate craniofacial and hindbrain patterning. Segmental control of Hoxa2 expression is crucial to its function and several studies have highlighted transcriptional regulatory elements governing its activity in distinct rhombomeres. Here, we identify a putative Hox-Pbx responsive cis-regulatory sequence, which resides in the coding sequence of Hoxa2 and is an important component of Hoxa2 regulation in rhombomere (r) 4. By using cell transfection and chromatin immunoprecipitation (ChIP) assays, we show that this regulatory sequence is responsive to paralogue group 1 and 2 Hox proteins and to their Pbx co-factors. Importantly, we also show that the Hox-Pbx element cooperates with a previously reported Hoxa2 r4 intronic enhancer and that its integrity is required to drive specific reporter gene expression in r4 upon electroporation in the chick embryo hindbrain. Thus, both intronic as well as exonic regulatory sequences are involved in Hoxa2 segmental regulation in the developing r4. Finally, we found that the Hox-Pbx exonic element is embedded in a larger 205-bp long ultraconserved genomic element (UCE) shared by all vertebrate genomes. In this respect, our data further support the idea that extreme conservation of UCE sequences may be the result of multiple superposed functional and evolutionary constraints.
机译:Hoxa2基因在脊椎动物颅面和后脑的模式中起基本作用。 Hoxa2表达的节段控制对其功能至关重要,一些研究强调了控制其在不同的菱形细胞中的活性的转录调控元件。在这里,我们确定了一个假定的Hox-Pbx响应性顺式调控序列,该序列位于Hoxa2的编码序列中,并且是菱形(r)4中Hoxa2调控的重要组成部分。通过使用细胞转染和染色质免疫沉淀(ChIP)分析,我们表明,该调控序列对旁系同源物1和2 Hox蛋白及其Pbx辅助因子有反应。重要的是,我们还表明,Hox-Pbx元件与先前报道的Hoxa2 r4内含子增强剂协同作用,并且在鸡胚后脑中进行电穿孔后,需要其完整性来驱动r4中的特定报告基因表达。因此,内含子和外显子调节序列都参与了发育中r4的Hoxa2节段调节。最后,我们发现Hox-Pbx外显子元件嵌入了所有脊椎动物基因组共有的更大205 bp长的超保守基因组元件(UCE)中。在这方面,我们的数据进一步支持了UCE序列的极端保守性可能是多重叠加的功能和进化约束的结果的想法。

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