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斑马鱼中hoxb3a和hoxb4a的保守共调控及启动子共享

Conserved co-regulation and promoter sharing of hoxb3a and hoxb4a in zebrafish.

作者信息

Hadrys Thorsten, Punnamoottil Beena, Pieper Mareike, Kikuta Hiroshi, Pezeron Guillaume, Becker Thomas S, Prince Victoria, Baker Robert, Rinkwitz Silke

机构信息

Department of Physiology and Neuroscience, NYU Medical School, New York, NY 10016, USA.

出版信息

Dev Biol. 2006 Sep 1;297(1):26-43. doi: 10.1016/j.ydbio.2006.04.446. Epub 2006 Apr 21.


DOI:10.1016/j.ydbio.2006.04.446
PMID:16860306
Abstract

The expression of zebrafish hoxb3a and hoxb4a has been found to be mediated through five transcripts, hoxb3a transcripts I-III and hoxb4a transcripts I-II, driven by four promoters. A "master" promoter, located about 2 kb downstream of hoxb5a, controls transcription of a pre-mRNA comprising exon sequences of both genes. This unique gene structure is proposed to provide a novel mechanism to ensure overlapping, tissue-specific expression of both genes in the posterior hindbrain and spinal cord. Transgenic approaches were used to analyze the functions of zebrafish hoxb3a/hoxb4a promoters and enhancer sequences containing regions of homology that were previously identified by comparative genomics. Two neural enhancers were shown to establish specific anterior expression borders within the hindbrain and mediate expression in defined neuronal populations derived from hindbrain rhombomeres (r) 5 to 8, suggesting a late role of the genes in neuronal cell lineage specification. Species comparison showed that the zebrafish hoxb3a r5 and r6 enhancer corresponded to a sequence within the mouse HoxA cluster controlling activity of Hoxa3 in r5 and r6, whereas a homologous region within the HoxB cluster activated Hoxb3 expression but limited to r5. We conclude that the similarity of hoxb3a/Hoxa3 regulatory mechanisms reflect the shared descent of both genes from a single ancestral paralog group 3 gene.

摘要

已发现斑马鱼hoxb3a和hoxb4a的表达由四个启动子驱动的五个转录本介导,即hoxb3a转录本I-III和hoxb4a转录本I-II。一个“主”启动子位于hoxb5a下游约2 kb处,控制包含两个基因外显子序列的前体mRNA的转录。这种独特的基因结构被认为提供了一种新机制,以确保这两个基因在后脑后部和脊髓中重叠的、组织特异性的表达。采用转基因方法分析斑马鱼hoxb3a/hoxb4a启动子以及含有先前通过比较基因组学鉴定的同源区域的增强子序列的功能。两个神经增强子显示在后脑内建立特定的前侧表达边界,并介导来自后脑菱脑节(r)5至8的特定神经元群体中的表达,表明这些基因在神经元细胞谱系特化中起后期作用。物种比较表明,斑马鱼hoxb3a的r5和r6增强子对应于小鼠HoxA簇中控制r5和r6中Hoxa3活性的一个序列,而HoxB簇中的一个同源区域激活Hoxb3表达但仅限于r5。我们得出结论,hoxb3a/Hoxa3调控机制的相似性反映了这两个基因来自单个祖先旁系同源基因群3基因的共同起源。

相似文献

[1]
Conserved co-regulation and promoter sharing of hoxb3a and hoxb4a in zebrafish.

Dev Biol. 2006-9-1

[2]
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J Exp Zool B Mol Dev Evol. 2004-3-15

[3]
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Dev Biol. 2002-6-1

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[10]
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[4]
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BMC Genomics. 2008-10-3

[5]
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[6]
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Genome Biol. 2007

[7]
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[8]
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