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Developmental and physiologic roles of the nuclear receptor steroidogenic factor-1 in the reproductive system.
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2
DNA binding and transcriptional repression by DAX-1 blocks steroidogenesis.DAX-1的DNA结合与转录抑制作用会阻断类固醇生成。
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Transcriptional activation and repression by RORalpha, an orphan nuclear receptor required for cerebellar development.
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The activation function-2 hexamer of steroidogenic factor-1 is required, but not sufficient for potentiation by SRC-1.类固醇生成因子-1的激活功能-2六聚体是必需的,但对于SRC-1的增强作用并不充分。
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Nuclear receptor steroidogenic factor 1 directs embryonic stem cells toward the steroidogenic lineage.核受体类固醇生成因子1引导胚胎干细胞走向类固醇生成谱系。
Mol Cell Biol. 1997 Jul;17(7):3997-4006. doi: 10.1128/MCB.17.7.3997.
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The mouse adrenocorticotropin receptor gene: cloning and characterization of its promoter and evidence for a role for the orphan nuclear receptor steroidogenic factor 1.小鼠促肾上腺皮质激素受体基因:其启动子的克隆与特性分析以及孤儿核受体类固醇生成因子1作用的证据
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7
Gene silencing by chicken ovalbumin upstream promoter-transcription factor I (COUP-TFI) is mediated by transcriptional corepressors, nuclear receptor-corepressor (N-CoR) and silencing mediator for retinoic acid receptor and thyroid hormone receptor (SMRT).鸡卵清蛋白上游启动子转录因子I(COUP-TFI)介导的基因沉默是由转录共抑制因子、核受体共抑制因子(N-CoR)以及维甲酸受体和甲状腺激素受体沉默介质(SMRT)介导的。
Mol Endocrinol. 1997 Jun;11(6):714-24. doi: 10.1210/mend.11.6.0002.
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The nuclear receptor SF-1 mediates sexually dimorphic expression of Mullerian Inhibiting Substance, in vivo.核受体SF-1在体内介导苗勒管抑制物质的性别二态性表达。
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10
Nuclear receptor repression mediated by a complex containing SMRT, mSin3A, and histone deacetylase.由包含SMRT、mSin3A和组蛋白去乙酰化酶的复合物介导的核受体抑制作用。
Cell. 1997 May 2;89(3):373-80. doi: 10.1016/s0092-8674(00)80218-4.

核受体DAX-1将核受体共抑制因子N-CoR募集至类固醇生成因子1。

Nuclear receptor DAX-1 recruits nuclear receptor corepressor N-CoR to steroidogenic factor 1.

作者信息

Crawford P A, Dorn C, Sadovsky Y, Milbrandt J

机构信息

Department of Pathology, Washington University School of Medicine, St. Louis, Missouri 63110, USA.

出版信息

Mol Cell Biol. 1998 May;18(5):2949-56. doi: 10.1128/MCB.18.5.2949.

DOI:10.1128/MCB.18.5.2949
PMID:9566914
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC110674/
Abstract

The orphan nuclear receptor steroidogenic factor 1 (SF-1) is a critical developmental regulator in the urogenital ridge, because mice targeted for disruption of the SF-1 gene lack adrenal glands and gonads. SF-1 was recently shown to interact with DAX-1, another orphan receptor whose tissue distribution overlaps that of SF-1. Naturally occurring loss-of-function mutations of the DAX-1 gene cause the human disorder X-linked adrenal hypoplasia congenita (AHC), which resembles the phenotype of SF-1-deficient mice. Paradoxically, however, DAX-1 represses the transcriptional activity of SF-1, and AHC mutants of DAX-1 lose repression function. To further investigate these findings, we characterized the interaction between SF-1 and DAX-1 and found that their interaction indeed occurs through a repressive domain within the carboxy terminus of SF-1. Furthermore, we demonstrate that DAX-1 recruits the nuclear receptor corepressor N-CoR to SF-1, whereas naturally occurring AHC mutations of DAX-1 permit the SF-1-DAX-1 interaction, but markedly diminish corepressor recruitment. Finally, the interaction between DAX-1 and N-CoR shares similarities with that of the nuclear receptor RevErb and N-CoR, because the related corepressor SMRT was not efficiently recruited by DAX-1. Therefore, DAX-1 can serve as an adapter molecule that recruits nuclear receptor corepressors to DNA-bound nuclear receptors like SF-1, thereby extending the range of corepressor action.

摘要

孤儿核受体类固醇生成因子1(SF-1)是泌尿生殖嵴中一种关键的发育调节因子,因为靶向破坏SF-1基因的小鼠缺乏肾上腺和性腺。最近发现SF-1与另一种孤儿受体DAX-1相互作用,DAX-1的组织分布与SF-1重叠。DAX-1基因的自然发生的功能丧失突变导致人类疾病X连锁先天性肾上腺发育不全(AHC),其类似于SF-1缺陷小鼠的表型。然而,矛盾的是,DAX-1抑制SF-1的转录活性,而DAX-1的AHC突变体失去抑制功能。为了进一步研究这些发现,我们对SF-1和DAX-1之间的相互作用进行了表征,发现它们的相互作用确实通过SF-1羧基末端的一个抑制结构域发生。此外,我们证明DAX-1将核受体共抑制因子N-CoR招募到SF-1上,而DAX-1的自然发生的AHC突变允许SF-1-DAX-1相互作用,但显著减少共抑制因子的招募。最后,DAX-1和N-CoR之间的相互作用与核受体RevErb和N-CoR的相互作用具有相似性,因为相关的共抑制因子SMRT不能被DAX-1有效招募。因此,DAX-1可以作为一种衔接分子,将核受体共抑制因子招募到与DNA结合的核受体如SF-1上,从而扩展共抑制因子的作用范围。