加压器
生物
糖皮质激素受体
转录因子
糖皮质激素
结合位点
螺旋(腹足类)
生物化学
氨基酸
抑制因子
立体化学
受体
生物物理学
基因
化学
内分泌学
蜗牛
生态学
作者
Jungki Min,L. Perera,J.M. Krahn,Christine M. Jewell,A.F. Moon,John A. Cidlowski,Lars C. Pedersen
摘要
Glucocorticoid receptor β (GRβ) is associated with glucocorticoid resistance via dominant negative regulation of GRα. To better understand how GRβ functions as a dominant negative inhibitor of GRα at a molecular level, we determined the crystal structure of the ligand binding domain of GRβ complexed with the antagonist RU-486. The structure reveals that GRβ binds RU-486 in the same ligand binding pocket as GRα, and the unique C-terminal amino acids of GRβ are mostly disordered. Binding energy analysis suggests that these C-terminal residues of GRβ do not contribute to RU-486 binding. Intriguingly, the GRβ/RU-486 complex binds corepressor peptide with affinity similar to that of a GRα/RU-486 complex, despite the lack of helix 12. Our biophysical and biochemical analyses reveal that in the presence of RU-486, GRβ is found in a conformation that favors corepressor binding, potentially antagonizing GRα function. This study thus presents an unexpected molecular mechanism by which GRβ could repress transcription.
科研通智能强力驱动
Strongly Powered by AbleSci AI