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甲状腺激素受体与垂体中类固醇受体辅激活因子-1的特异性相互作用。

Thyroid hormone receptor-specific interactions with steroid receptor coactivator-1 in the pituitary.

作者信息

Sadow Peter M, Koo Eugene, Chassande Olivier, Gauthier Karine, Samarut Jacques, Xu Jianming, O'Malley Bert W, Seo Hisao, Murata Yoshiharu, Weiss Roy E

机构信息

Department of Medicine, University of Chicago, Illinois, USA.

出版信息

Mol Endocrinol. 2003 May;17(5):882-94. doi: 10.1210/me.2002-0174. Epub 2003 Feb 6.

Abstract

Steroid receptor coactivator-1 (SRC-1) is a transcription cofactor that enhances the hormone-dependent action mediated by the thyroid hormone (TH) receptor (TR) as well as other nuclear receptors. However, it is not known whether the SRC-1-mediated activation of TH-regulated gene transcription is TR isoform specific in the pituitary. We generated mice that were deficient in TRalpha and SRC-1 (TRalpha(0/0)SRC-1(-/-)), as well in TRbeta and SRC-1 (TRbeta(-/-)SRC-1(-/-)), and thyroid function tests and effects of TH deprivation and TH treatment were compared with wild-type mice or mice with deletion of either TRs or SRC-1 alone. We have shown that 1) TRbeta(-/-)SRC-1(-/-) mice demonstrate more severe TH resistance than either the SRC-1(-/-) or TRbeta(-/-) mice; the additive effect indicates that SRC-1 has an independent role in TH action over that of TRbeta; 2) SRC-1 facilitates TRbeta and TRalpha-mediated down-regulation of TSH, as TRalpha(0/0)SRC-1(-/-) mice demonstrate TH resistance rather than hypersensitivity as seen in TRalpha(0/0)mice; and 3) a compensatory increase in SRC-1 expression is associated with the TH hypersensitivity seen in TRalpha-deficient animals. We conclude that SRC-1 action in the pituitary mediates TH action via specific TR subtypes.

摘要

类固醇受体辅激活因子-1(SRC-1)是一种转录辅因子,可增强由甲状腺激素(TH)受体(TR)以及其他核受体介导的激素依赖性作用。然而,SRC-1介导的TH调节基因转录激活在垂体中是否具有TR亚型特异性尚不清楚。我们培育了TRα和SRC-1双缺陷(TRα(0/0)SRC-1(-/-))以及TRβ和SRC-1双缺陷(TRβ(-/-)SRC-1(-/-))的小鼠,并将甲状腺功能测试以及TH剥夺和TH治疗的效果与野生型小鼠或单独缺失TRs或SRC-1的小鼠进行了比较。我们发现:1)TRβ(-/-)SRC-1(-/-)小鼠表现出比SRC-1(-/-)或TRβ(-/-)小鼠更严重的TH抵抗;这种累加效应表明SRC-1在TH作用中具有独立于TRβ的作用;2)SRC-1促进TRβ和TRα介导的促甲状腺激素(TSH)下调,因为TRα(0/0)SRC-1(-/-)小鼠表现出TH抵抗而非TRα(0/0)小鼠中所见的甲状腺功能亢进;3)SRC-1表达的代偿性增加与TRα缺陷动物中所见的TH超敏反应相关。我们得出结论,SRC-1在垂体中的作用通过特定的TR亚型介导TH作用。

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