Structural Analysis on the Pathologic Mutant Glucocorticoid Receptor Ligand-Binding Domains.

Q Biochemistry, Genetics and Molecular Biology
D. Hurt, S. Suzuki, T. Mayama, E. Charmandari, T. Kino
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引用次数: 18

Abstract

Glucocorticoid receptor (GR) gene mutations may cause familial or sporadic generalized glucocorticoid resistance syndrome. Most of the missense forms distribute in the ligand-binding domain and impair its ligand-binding activity and formation of the activation function (AF)-2 that binds LXXLL motif-containing coactivators. We performed molecular dynamics simulations to ligand-binding domain of pathologic GR mutants to reveal their structural defects. Several calculated parameters including interaction energy for dexamethasone or the LXXLL peptide indicate that destruction of ligand-binding pocket (LBP) is a primary character. Their LBP defects are driven primarily by loss/reduction of the electrostatic interaction formed by R611 and T739 of the receptor to dexamethasone and a subsequent conformational mismatch, which deacylcortivazol resolves with its large phenylpyrazole moiety and efficiently stimulates transcriptional activity of the mutant receptors with LBP defect. Reduced affinity of the LXXLL peptide to AF-2 is caused mainly by disruption of the electrostatic bonds to the noncore leucine residues of this peptide that determine the peptide's specificity to GR, as well as by reduced noncovalent interaction against core leucines and subsequent exposure of the AF-2 surface to solvent. The results reveal molecular defects of pathologic mutant receptors and provide important insights to the actions of wild-type GR.
病理性突变糖皮质激素受体配体结合域的结构分析。
糖皮质激素受体(GR)基因突变可引起家族性或散发的广泛性糖皮质激素抵抗综合征。大多数错义形式分布在配体结合域,损害其配体结合活性和与LXXLL基序共激活子结合的激活功能(AF)-2的形成。我们对病理性GR突变体的配体结合域进行了分子动力学模拟,以揭示其结构缺陷。包括地塞米松或LXXLL肽的相互作用能在内的几个计算参数表明,配体结合袋(LBP)的破坏是其主要特征。它们的LBP缺陷主要是由受体的R611和T739与地塞米松形成的静电相互作用的丢失/减少以及随后的构象错配驱动的,去酰基cortivazol用其大的苯吡唑片段解决了这一问题,并有效地刺激了LBP缺陷突变受体的转录活性。LXXLL肽对AF-2的亲和力降低主要是由于与该肽的非核心亮氨酸残基(决定该肽对GR的特异性)的静电键被破坏,以及与核心亮氨酸的非共价相互作用减少以及随后将AF-2表面暴露于溶剂中。这些结果揭示了病理突变受体的分子缺陷,为野生型GR的作用提供了重要的见解。
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来源期刊
Molecular endocrinology
Molecular endocrinology 医学-内分泌学与代谢
CiteScore
3.49
自引率
0.00%
发文量
0
审稿时长
12 months
期刊介绍: Molecular Endocrinology provides a forum for papers devoted to describing molecular mechanisms by which hormones and related compounds regulate function. It has quickly achieved a reputation as a high visibility journal with very rapid communication of cutting edge science: the average turnaround time is 28 days from manuscript receipt to first decision, and accepted manuscripts are published online within a week through Rapid Electronic Publication. In the 2008 Journal Citation Report, Molecular Endocrinology is ranked 16th out of 93 journals in the Endocrinology and Metabolism category, with an Impact Factor of 5.389.
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