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甲状腺激素和视黄酸受体对基因表达调控的一些新变化。

Some new twists in the regulation of gene expression by thyroid hormone and retinoic acid receptors.

作者信息

Glass C K

机构信息

Department of Medicine, University of California, San Diego, La Jolla 92093-0651, USA.

出版信息

J Endocrinol. 1996 Sep;150(3):349-57. doi: 10.1677/joe.0.1500349.

Abstract

Recent studies indicate that heterodimeric nuclear receptors utilize several novel mechanisms for increasing the complexity of transcriptional responses to hormonal stimuli. By binding as heterodimers, these receptors can potentially respond to more than one activating ligand. Allosteric interactions between the ligand binding domains of RXR and its heterodimeric partners regulate the binding of RXR ligands, resulting in either selective or dual transcriptional responses. Regulation of the relative levels of expression of different heterodimeric partners that permit signaling through RXR is likely further to expand the patterns of transcriptional responses that can occur through a given response element. Heterodimeric nuclear receptors also bind to asymmetric response elements with specific polarities that result from the formation of cooperative interfaces between DNA binding domains. The DNA binding interface serves to determine the response element specificity of different heterodimers based on the spacing between half sites. The specific polarity of DNA binding has also been shown to provide a mechanism for regulating the transcriptional responses of retinoic acid receptors to activating ligands through the differential control of co-repressor interactions. The identification and characterization of co-activator and co-repressor molecules is likely to provide a very interesting next chapter to the mechanisms of steroid hormone action.

摘要

最近的研究表明,异二聚体核受体利用几种新机制来增加对激素刺激的转录反应的复杂性。通过以异二聚体形式结合,这些受体可能对不止一种激活配体产生反应。RXR与其异二聚体伙伴的配体结合域之间的变构相互作用调节RXR配体的结合,从而产生选择性或双重转录反应。调节不同异二聚体伙伴的相对表达水平,使其能够通过RXR进行信号传导,可能会进一步扩大通过给定反应元件可能发生的转录反应模式。异二聚体核受体还以特定极性结合不对称反应元件,这种极性是由DNA结合域之间形成的协同界面导致的。DNA结合界面用于根据半位点之间的间距确定不同异二聚体的反应元件特异性。DNA结合的特定极性还被证明通过对共抑制因子相互作用的差异控制,为调节视黄酸受体对激活配体的转录反应提供了一种机制。共激活因子和共抑制因子分子的鉴定和表征可能会为类固醇激素作用机制开启非常有趣的新篇章。

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