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类固醇受体招募LXXLL和FXXLF基序中的静电调制。

Electrostatic modulation in steroid receptor recruitment of LXXLL and FXXLF motifs.

作者信息

He Bin, Wilson Elizabeth M

机构信息

Laboratories for Reproductive Biology, Department of Biochemistry and Biophysics, University of North Carolina, 374 Medical Sciences Research Building, Chapel Hill, NC 27599-7500, USA.

出版信息

Mol Cell Biol. 2003 Mar;23(6):2135-50. doi: 10.1128/MCB.23.6.2135-2150.2003.

DOI:10.1128/MCB.23.6.2135-2150.2003
PMID:12612084
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC149467/
Abstract

Coactivator recruitment by activation function 2 (AF2) in the steroid receptor ligand binding domain takes place through binding of an LXXLL amphipathic alpha-helical motif at the AF2 hydrophobic surface. The androgen receptor (AR) and certain AR coregulators are distinguished by an FXXLF motif that interacts selectively with the AR AF2 site. Here we show that LXXLL and FXXLF motif interactions with steroid receptors are modulated by oppositely charged residues flanking the motifs and charge clusters bordering AF2 in the ligand binding domain. An increased number of charged residues flanking AF2 in the ligand binding domain complement the two previously characterized charge clamp residues in coactivator recruitment. The data suggest a model whereby coactivator recruitment to the receptor AF2 surface is initiated by complementary charge interactions that reflect a reversal of the acidic activation domain-coactivator interaction model.

摘要

类固醇受体配体结合域中的激活功能2(AF2)通过LXXLL两亲性α-螺旋基序在AF2疏水表面的结合来招募共激活因子。雄激素受体(AR)和某些AR共调节因子的特征是具有一个FXXLF基序,该基序与AR AF2位点选择性相互作用。在这里,我们表明LXXLL和FXXLF基序与类固醇受体的相互作用受到基序侧翼带相反电荷的残基以及配体结合域中与AF2相邻的电荷簇的调节。配体结合域中AF2侧翼带电荷残基数量的增加补充了共激活因子招募中两个先前表征的电荷钳制残基。这些数据提出了一个模型,即通过互补电荷相互作用启动共激活因子向受体AF2表面的招募,这反映了酸性激活域 - 共激活因子相互作用模型的逆转。

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