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配体结合的视黄醇X受体(RXR)在胚胎发生过程中可介导类视黄醇信号转导。

Ligand-bound RXR can mediate retinoid signal transduction during embryogenesis.

作者信息

Lu H C, Eichele G, Thaller C

机构信息

V. and M. McLean Department of Biochemistry, Baylor College of Medicine, Houston, Texas 77030, USA.

出版信息

Development. 1997 Jan;124(1):195-203. doi: 10.1242/dev.124.1.195.

DOI:10.1242/dev.124.1.195
PMID:9006080
Abstract

Retinoids regulate various aspects of vertebrate development through the action of two types of receptors, the retinoic acid receptors (RARs) and the retinoid-X-receptors (RXRs). Although RXRs bind 9-cis-retinoic acid (9cRA) with high affinity, in vitro experiments suggest that RXRs are for the most part not liganded, but serve as auxiliary factors forming heterodimers with liganded partner receptors such as RAR. Here we have used RXR- and RAR-specific ligands 4-[1-(3,5,5,8,8-pentamethyl-5,6,7,8-tetrahydro-2-napthyl)ethenyl]b enzoic acid (LG69) and (E)-4-[2-(5,5,8,8-tetramethyl-5,6,7,8-tetrahydro-2-naphthalenyl)-1-prope nyl]benzoic acid (TTNPB), and show that, in the context of an embryo, liganded RXR can mediate retinoid signal transduction. This conclusion emerges from examining the induction of several retinoid-responsive genes in the limb bud (Hoxb-6/-8, RARbeta) and in the developing central nervous system (Hoxb-1, otx-2). RARbeta and Hoxb-1 genes were most effectively activated by a combination of TTNPB and LG69, suggesting that the activation of these genes benefits from the presence of ligand-bound RAR and ligand-bound RXR. Hoxb-6/-8 genes were most efficiently induced by LG69, suggesting that liganded RXR can activate these genes. The regulation of the expression of the otx-2 gene was complex; expression was repressed by TTNPB, but such repression was relieved when LG69 was provided together with TTNPB, suggesting that ligand-bound RXR can overcome repression of transcription exerted by liganded RAR. Based on these findings, we propose that in our experimental system in which ligands are provided exogenously, transcriptional regulation of several genes involves liganded RXR.

摘要

维甲酸通过两种受体,即维甲酸受体(RARs)和维甲酸X受体(RXRs)的作用来调节脊椎动物发育的各个方面。尽管RXRs与9-顺式维甲酸(9cRA)具有高亲和力结合,但体外实验表明,在大多数情况下RXRs并未与配体结合,而是作为辅助因子与诸如RAR等与配体结合的伙伴受体形成异二聚体。在此,我们使用了RXR和RAR特异性配体4-[1-(3,5,5,8,8-五甲基-5,6,7,8-四氢-2-萘基)乙烯基]苯甲酸(LG69)和(E)-4-[2-(5,5,8,8-四甲基-5,6,7,8-四氢-2-萘基)-1-丙烯基]苯甲酸(TTNPB),并表明,在胚胎环境中,与配体结合的RXR能够介导维甲酸信号转导。这一结论来自于对肢芽(Hoxb-6/-8、RARβ)和发育中的中枢神经系统(Hoxb-1、otx-2)中几个维甲酸反应性基因诱导情况的研究。RARβ和Hoxb-1基因最有效地被TTNPB和LG69的组合激活,这表明这些基因的激活得益于与配体结合的RAR和与配体结合的RXR的存在。Hoxb-6/-8基因最有效地被LG69诱导,这表明与配体结合的RXR能够激活这些基因。otx-2基因表达的调控较为复杂;TTNPB可抑制其表达,但当LG69与TTNPB一起提供时,这种抑制作用得到缓解,这表明与配体结合的RXR能够克服与配体结合的RAR对转录的抑制作用。基于这些发现,我们提出,在我们外源提供配体的实验系统中,几个基因的转录调控涉及与配体结合的RXR。

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