首页> 美国卫生研究院文献>Biochemical Journal >Single thyroid hormone receptor monomers are competent for co-activator-mediated transactivation.
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Single thyroid hormone receptor monomers are competent for co-activator-mediated transactivation.

机译:单个甲状腺激素受体单体可胜任辅激活子介导的反式激活。

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摘要

Thyroid hormone receptor (T(3)R) belongs to the superfamily of nuclear receptors containing highly related transcription factors that transform an incoming signal in the form of a lipophilic hormone into an activation of the basal transcriptional machinery. Like many other nuclear receptors, T(3)R acts preferentially as a heterodimer with retinoid X receptor (RXR) but it also has the unique property of binding as a monomer to DNA. This study demonstrates that T(3)R monomers bind preferentially to AGGTCA binding motifs and are able to co-exist with T(3)R-RXR heterodimers in the presence of limiting amounts of RXR. DNA-bound T(3)R monomers efficiently contact all three members of the p160 co-activator family, which in turn boost T(3)R monomer-mediated transactivation. In solution T(3)R monomers take only one agonistic conformation (c2(LPD)), whereas bound to DNA they also stabilize, like T(3)R-RXR heterodimers, a second agonistic conformation (c1(LPD)). Conformation c2(LPD) seems to be of lower ligand sensitivity (10 nM), whereas, both in T(3)R-RXR heterodimers and in DNA-bound T(3)R monomers, c1(LPD) is already activated at a ligand concentration of 1 nM. Taken together, these results suggest that single T(3)R monomers are fully competent for ligand-induced transactivation and that their role in gene regulation by thyroid hormone might have been underestimated.
机译:甲状腺激素受体(T(3)R)属于核受体的超家族,其包含高度相关的转录因子,这些转录因子将以亲脂性激素形式出现的信号转化为基础转录机制的激活。像许多其他核受体一样,T(3)R优先充当类视黄醇X受体(RXR)的异二聚体,但它也具有作为单体与DNA结合的独特特性。这项研究表明,T(3)R单体优先结合AGGTCA结合基序,并能够在有限量的RXR存在下与T(3)R-RXR异二聚体共存。与DNA结合的T(3)R单体有效接触p160共激活子家族的所有三个成员,这反过来又增强了T(3)R单体介导的反式激活。在溶液中,T(3)R单体仅具有一种激动性构象(c2(LPD)),而与DNA结合时,它们也像T(3)R-RXR异二聚体一样稳定于第二种激动性构象(c1(LPD))。构象c2(LPD)似乎具有较低的配体敏感性(10 nM),而在T(3)R-RXR异二聚体和与DNA结合的T(3)R单体中,c1(LPD)均已被激活。配体浓度为1 nM。综上所述,这些结果表明单个T(3)R单体完全能够胜任配体诱导的反式激活,并且它们在甲状腺激素基因调控中的作用可能被低估了。

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