WDR5 Binding to Histone Serotonylation Is Driven by an Edge–Face Aromatic Interaction with Unexpected Electrostatic Effects

化学 GSM演进的增强数据速率 面子(社会学概念) 组蛋白 计算化学 立体化学 生物化学 人工智能 基因 计算机科学 社会科学 社会学
作者
Christopher R. Travis,Hanne C. Henriksen,Jake R. Wilkinson,Noah K. Schomburg,Joseph W. Treacy,K.M. Kean,K. N. Houk,Marcey L. Waters
出处
期刊:Journal of the American Chemical Society [American Chemical Society]
被引量:2
标识
DOI:10.1021/jacs.4c07277
摘要

Histone serotonylation has emerged as a key post-translational modification. WDR5 preferentially binds to serotonylated histone 3 (H3), and this binding event has been associated with tumorigenesis. Herein, we utilize genetic code expansion, structure-activity relationship studies, and computation to study an edge-face aromatic interaction between WDR5 Phe149 and serotonin on H3 that is key to this protein-protein interaction. We find experimentally that this edge-face aromatic interaction is unaffected by modulating the electrostatics of the face component but is weakened by electron-withdrawing substituents on the edge component. Overall, these results elucidate that this interaction is governed by van der Waals forces as well as electrostatics of the edge ring, a result that clarifies discrepancies among previous theoretical models and model system studies of this interaction type. This is the first evaluation of the driving force of an edge-face aromatic interaction at a protein-protein interface and provides a key benchmark for the nature of these understudied interactions that are abundant in the proteome.
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