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Dax-1(X染色体剂量敏感性性反转-先天性肾上腺发育不全关键区域,基因1)基因转录在雌性性腺发育过程中受Wnt4调控。

Dax-1 (dosage-sensitive sex reversal-adrenal hypoplasia congenita critical region on the X chromosome, gene 1) gene transcription is regulated by wnt4 in the female developing gonad.

作者信息

Mizusaki Hirofumi, Kawabe Ken, Mukai Tokuo, Ariyoshi Etsuko, Kasahara Megumi, Yoshioka Hidefumi, Swain Amanda, Morohashi Ken-Ichirou

机构信息

Department of Developmental Biology, National Institute for Basic Biology, Myodaiji-cho, Okazaki 444-8585, Japan.

出版信息

Mol Endocrinol. 2003 Apr;17(4):507-19. doi: 10.1210/me.2002-0362. Epub 2003 Jan 23.

DOI:10.1210/me.2002-0362
PMID:12554773
Abstract

Dax-1 [dosage-sensitive sex reversal-adrenal hypoplasia congenita critical region on the X chromosome, gene 1 (NR0B1)] is an orphan nuclear receptor acting as a suppressor of Ad4 binding protein/steroidogenic factor 1 [Ad4BP/SF-1 (NR5A1)] and as an anti-Sry factor in the process of gonadal sex differentiation. The roles of these nuclear receptors in the differentiation of the gonads and the adrenal cortex have been established through studies of the mutant phenotype in both mice and humans. However, the mechanisms underlying transcriptional regulation of these genes remain largely unknown. Here, we examined the relationship between Dax-1 gene transcription and the Wnt4 pathway. Reporter gene analysis revealed that Dax-1 gene transcription was activated by beta-catenin, a key signal-transducing protein in the Wnt pathway, acting in synergy with Ad4BP/SF-1. Interaction between beta-catenin and Ad4BP/SF-1 was observed using yeast two-hybrid and in vitro pull-down assays. The region of Ad4BP/SF-1 essential for this interaction consists of an acidic amino acid cluster, which resides in the first helix of the ligand-binding domain. Mutation of the amino acid cluster impaired transcriptional activation of Dax-1 as well as interaction of Ad4BP/SF-1 with beta-catenin. These results were supported by in vivo observations using Wnt4 gene-disrupted mice, in which Dax-1 gene expression was decreased significantly in sexually differentiating female gonads. We thus conclude that Wnt4 signaling mediates the increased expression of Dax-1 as the ovary becomes sexually differentiated.

摘要

Dax-1[X染色体剂量敏感性性别反转-先天性肾上腺发育不全关键区域,基因1(NR0B1)]是一种孤儿核受体,在性腺性别分化过程中作为Ad4结合蛋白/类固醇生成因子1[Ad4BP/SF-1(NR5A1)]的抑制因子以及抗Sry因子发挥作用。通过对小鼠和人类突变表型的研究,已经明确了这些核受体在性腺和肾上腺皮质分化中的作用。然而,这些基因转录调控的潜在机制在很大程度上仍然未知。在此,我们研究了Dax-1基因转录与Wnt4信号通路之间的关系。报告基因分析显示,Dax-1基因转录由β-连环蛋白激活,β-连环蛋白是Wnt信号通路中的关键信号转导蛋白,与Ad4BP/SF-1协同作用。使用酵母双杂交和体外下拉试验观察到β-连环蛋白与Ad4BP/SF-1之间的相互作用。Ad4BP/SF-1中对于这种相互作用至关重要的区域由一个酸性氨基酸簇组成,该簇位于配体结合域的第一个螺旋中。氨基酸簇的突变损害了Dax-1的转录激活以及Ad4BP/SF-1与β-连环蛋白的相互作用。使用Wnt4基因敲除小鼠的体内观察结果支持了这些结果,在这些小鼠中,在性别分化的雌性性腺中Dax-1基因表达显著降低。因此,我们得出结论,随着卵巢开始性别分化,Wnt4信号介导了Dax-1表达的增加。

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