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鉴定小鼠糖皮质激素受体tau 2区域中有助于激素结合和转录激活的氨基酸。

Identification of amino acids in the tau 2-region of the mouse glucocorticoid receptor that contribute to hormone binding and transcriptional activation.

作者信息

Milhon J, Lee S, Kohli K, Chen D, Hong H, Stallcup M R

机构信息

Department of Pathology, University of Southern California, Los Angeles 90033, USA.

出版信息

Mol Endocrinol. 1997 Nov;11(12):1795-805. doi: 10.1210/mend.11.12.0018.

Abstract

The tau 2-region of steroid hormone receptors is a highly conserved region located at the extreme N-terminal end of the hormone-binding domain. A protein fragment encoding tau 2 has been shown to function as an independent transcriptional activation domain; however, because this region is essential for hormone binding, it has been difficult to determine whether the tau 2-region also contributes to the transactivation function of intact steroid receptors. In this study a series of amino acid substitutions were engineered at conserved positions in the tau 2-region of the mouse glucocorticoid receptor (mGR, amino acids 533-562) to map specific amino acid residues that contribute to the hormone-binding function, transcriptional activation, or both. Substitution of alanine or glycine for some amino acids (mutations E546G, P547A, and D555A) reduced or eliminated hormone binding, but the transactivation function of the intact GR and/or the minimum tau 2-fragment was unaffected for each of these mutants. Substitution of alanine for amino acid S561 reduced transactivation activity in the intact GR and the minimum tau 2-fragment but had no effect on hormone binding. The single mutation L550A and the double amino acid substitution L541G+L542G affected both hormone binding and transactivation. The fact that the S561A and L550A substitutions each caused a loss of transactivation activity in the minimum tau 2-fragment and the full-length GR indicated that the tau 2-region does contribute to the overall transactivation function of the full-length GR. Overall, the N-terminal portion of the tau 2-region (mGR 541-547) was primarily involved in hormone binding, whereas the C-terminal portion of the tau 2-region (mGR 548-561) was primarily involved in transactivation.

摘要

类固醇激素受体的tau 2区域是一个高度保守的区域,位于激素结合域的最N端。编码tau 2的蛋白质片段已被证明可作为一个独立的转录激活域发挥作用;然而,由于该区域对于激素结合至关重要,因此很难确定tau 2区域是否也对完整类固醇受体的反式激活功能有贡献。在本研究中,在小鼠糖皮质激素受体(mGR,氨基酸533 - 562)的tau 2区域的保守位置设计了一系列氨基酸替换,以确定对激素结合功能、转录激活或两者都有贡献的特定氨基酸残基。用丙氨酸或甘氨酸替换某些氨基酸(突变E546G、P547A和D555A)会降低或消除激素结合,但对于这些突变体中的每一个,完整GR和/或最小tau 2片段的反式激活功能均未受影响。用丙氨酸替换氨基酸S561会降低完整GR和最小tau 2片段中的反式激活活性,但对激素结合没有影响。单突变L550A和双氨基酸替换L541G + L542G对激素结合和反式激活均有影响。S561A和L550A替换均导致最小tau 2片段和全长GR中反式激活活性丧失,这一事实表明tau 2区域确实对全长GR的整体反式激活功能有贡献。总体而言,tau 2区域的N端部分(mGR 541 - 547)主要参与激素结合,而tau 2区域的C端部分(mGR 548 - 561)主要参与反式激活。

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