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胎儿肾上腺发育过程中Ad4BP/SF-1基因转录的两步调节:由Hox-Pbx1-Prep1复合体启动并通过Ad4BP/SF-1自身调节维持。

Two-step regulation of Ad4BP/SF-1 gene transcription during fetal adrenal development: initiation by a Hox-Pbx1-Prep1 complex and maintenance via autoregulation by Ad4BP/SF-1.

作者信息

Zubair Mohamad, Ishihara Satoru, Oka Sanae, Okumura Katsuzumi, Morohashi Ken-ichirou

机构信息

Division of Sex Differentiation, National Institute for Basic Biology, Myodaiji-cho, Okazaki 444-8787, Japan.

出版信息

Mol Cell Biol. 2006 Jun;26(11):4111-21. doi: 10.1128/MCB.00222-06.

Abstract

The orphan nuclear receptor Ad4BP/SF-1 (adrenal 4 binding protein/steroidogenic factor 1) is essential for the proper development and function of reproductive and steroidogenic tissues. Although the expression of Ad4BP/SF-1 is specific for those tissues, the mechanisms underlying this tissue-specific expression remain unknown. In this study, we used transgenic mouse assays to examine the regulation of the tissue-specific expression of Ad4BP/SF-1. An investigation of the entire Ad4BP/SF-1 gene locus revealed a fetal adrenal enhancer (FAdE) in intron 4 containing highly conserved binding sites for Pbx-Prep, Pbx-Hox, and Ad4BP/SF-1. Transgenic assays revealed that the Ad4 sites, together with Ad4BP/SF-1, develop an autoregulatory loop and thereby maintain transcription, while the Pbx/Prep and Pbx/Hox sites initiate transcription prior to the establishment of the autoregulatory loop. Indeed, a limited number of Hox family members were found to be expressed in the adrenal primordia. Whether a true fetal-type adrenal cortex is present in mice remained controversial, and this argument was complicated by the postnatal development of the so-called X zone. Using transgenic mice with lacZ driven by the FAdE, we clearly identified a fetal adrenal cortex in mice, and the X zone is the fetal adrenal cells accumulated at the juxtamedullary region after birth.

摘要

孤儿核受体Ad4BP/SF-1(肾上腺4结合蛋白/类固醇生成因子1)对于生殖和类固醇生成组织的正常发育及功能至关重要。尽管Ad4BP/SF-1的表达在这些组织中具有特异性,但其组织特异性表达的潜在机制仍不清楚。在本研究中,我们利用转基因小鼠实验来研究Ad4BP/SF-1组织特异性表达的调控。对整个Ad4BP/SF-1基因座的研究揭示了内含子4中的一个胎儿肾上腺增强子(FAdE),其含有Pbx-Prep、Pbx-Hox和Ad4BP/SF-1的高度保守结合位点。转基因实验表明,Ad4位点与Ad4BP/SF-1一起形成一个自调节环,从而维持转录,而Pbx/Prep和Pbx/Hox位点在自调节环建立之前启动转录。实际上,发现有限数量的Hox家族成员在肾上腺原基中表达。小鼠中是否存在真正的胎儿型肾上腺皮质仍存在争议,并且所谓X区的出生后发育使这一争论变得复杂。利用由FAdE驱动lacZ的转基因小鼠,我们清楚地在小鼠中鉴定出了胎儿肾上腺皮质,并且X区是出生后在近髓质区域积累的胎儿肾上腺细胞。

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