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ATOH7的分子特征与定位,ATOH7是一种人类无调蛋白同源物,在视网膜神经节细胞发育中具有预测作用。

Molecular characterization and mapping of ATOH7, a human atonal homolog with a predicted role in retinal ganglion cell development.

作者信息

Brown Nadean L, Dagenais Susan L, Chen Chuan-Min, Glaser Tom

机构信息

Department of Pediatrics at Children's Memorial Institute for Education and Research, Northwestern University Medical School, Chicago, Illinois 60614-3394, USA.

出版信息

Mamm Genome. 2002 Feb;13(2):95-101. doi: 10.1007/s00335-001-2101-3.

Abstract

The human ATOH7 gene encodes a basic helix-loop-helix (bHLH) transcription factor that is highly similar to Drosophila Atonal within the conserved bHLH domain. The ATOH7 coding region is contained within a single exon. We mapped ATOH7 to Chromosome (Chr) 10q21.3-22.1, a region syntenic to the segment of mouse Chr 10 where Atoh7 (formerly Math5) is located. The evolutionary relationship between ATOH7 and other atonal homologs was investigated using parsimony analysis. A direct comparison of ATH5/7 and ATH1 protein subgroups to Atonal also revealed a nonrandom distribution of amino acid changes across the bHLH domain, which may be related to their separate visual and proprioceptive sensory functions. Among bHLH genes, ATOH7 is most closely related to Atoh7. This sequence conservation extends significantly beyond the coding region. We define blocks of strong homology in flanking human and mouse genomic DNA, which are likely to include cis regulatory elements. Because targeted deletion of Atoh7 causes optic nerve agenesis in mice, we propose ATOH7 as a candidate for human optic nerve aplasia and related clinical syndromes.

摘要

人类ATOH7基因编码一种碱性螺旋-环-螺旋(bHLH)转录因子,在保守的bHLH结构域内与果蝇无调性蛋白高度相似。ATOH7编码区包含在一个外显子中。我们将ATOH7定位到染色体(Chr)10q21.3 - 22.1,该区域与小鼠Chr 10上Atoh7(以前称为Math5)所在的片段同线。使用简约分析研究了ATOH7与其他无调性同源物之间的进化关系。将ATH5/7和ATH1蛋白质亚组与无调性蛋白直接比较还发现,bHLH结构域上氨基酸变化的分布并非随机,这可能与其各自的视觉和本体感觉功能有关。在bHLH基因中,ATOH7与Atoh7关系最为密切。这种序列保守性显著延伸至编码区之外。我们确定了人类和小鼠侧翼基因组DNA中的强同源性区域,这些区域可能包含顺式调控元件。由于Atoh7的靶向缺失会导致小鼠视神经发育不全,我们提出ATOH7作为人类视神经发育不全及相关临床综合征的候选基因。

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