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指导糖皮质激素受体差异激活的动态变构通讯途径

Dynamic allosteric communication pathway directing differential activation of the glucocorticoid receptor.

作者信息

Köhler C, Carlström G, Gunnarsson A, Weininger U, Tångefjord S, Ullah V, Lepistö M, Karlsson U, Papavoine T, Edman K, Akke M

机构信息

Respiratory, Inflammation and Autoimmunity, Pharmaceutical Sciences, R&D, AstraZeneca, Gothenburg, Sweden.

Centre for Analysis and Synthesis, Department of Chemistry, Lund University, P.O. Box 124, 221 00 Lund, Sweden.

出版信息

Sci Adv. 2020 Jul 17;6(29):eabb5277. doi: 10.1126/sciadv.abb5277. eCollection 2020 Jul.

Abstract

Allosteric communication within proteins is a hallmark of biochemical signaling, but the dynamic transmission pathways remain poorly characterized. We combined NMR spectroscopy and surface plasmon resonance to reveal these pathways and quantify their energetics in the glucocorticoid receptor, a transcriptional regulator controlling development, metabolism, and immune response. Our results delineate a dynamic communication network of residues linking the ligand-binding pocket to the activation function-2 interface, where helix 12, a switch for transcriptional activation, exhibits ligand- and coregulator-dependent dynamics coupled to graded activation. The allosteric free energy responds to variations in ligand structure: subtle changes gradually tune allostery while preserving the transmission pathway, whereas substitution of the entire pharmacophore leads to divergent allosteric control by apparently rewiring the communication network. Our results provide key insights that should aid in the design of mechanistically differentiated ligands.

摘要

蛋白质内的变构通讯是生化信号传导的一个标志,但动态传递途径仍未得到充分表征。我们结合核磁共振光谱和表面等离子体共振来揭示这些途径,并量化它们在糖皮质激素受体中的能量学,糖皮质激素受体是一种控制发育、代谢和免疫反应的转录调节因子。我们的结果描绘了一个将配体结合口袋与激活功能-2界面连接起来的残基动态通讯网络,其中转录激活开关螺旋12表现出与分级激活相关的配体和共调节因子依赖性动态变化。变构自由能对配体结构的变化做出反应:细微变化逐渐调节变构作用,同时保留传递途径,而整个药效基团的取代则通过明显重新连接通讯网络导致不同的变构控制。我们的结果提供了关键见解,应有助于设计具有机制差异的配体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cd7e/7439413/23b8b5c14544/abb5277-F1.jpg

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