Identification of G-Quadruplex-Binding Protein from the Exploration of RGG Motif/G-Quadruplex Interactions

化学 亲缘关系 结合亲和力 G-四倍体 结构母题 结合选择性 血浆蛋白结合 生物化学 结合位点 绑定域 核糖开关 生物物理学 RNA结合蛋白 结合蛋白 核糖核酸 DNA 生物 基因 受体 非编码RNA
作者
Zhou-Li Huang,Jing Dai,Wen-Hua Luo,Xianggui Wang,Jia‐Heng Tan,Shuo‐Bin Chen,Zhi‐Shu Huang
出处
期刊:Journal of the American Chemical Society [American Chemical Society]
卷期号:140 (51): 17945-17955 被引量:97
标识
DOI:10.1021/jacs.8b09329
摘要

The arginine/glycine-rich region termed the RGG domain is usually found in G-quadruplex (G4)-binding proteins and is important in G4–protein interactions. Studies on the binding mechanism of RGG domains found that small segments (RGG motif) inside the domain contribute greatly to the G4 binding affinity. However, unlike the entire RGG domains that have been broadly explored, the role of the RGG motif remains obscure, with very limited study. Herein, to clarify the role of the RGG motif in G4–protein interactions, we systematically investigated the binding affinity and mode between RGG-motif peptides and G4s. The internal arrangement of RGG repeats and gap amino acids played a more crucial role in the G4-binding mechanism than a critical number of RGG repeats. Arginines and phenylalanines at the exact position of the RGG motif might enable additional hydrogen bonding and π-stacking interaction with nucleobases and strengthen the binding of G4. Impressively, proceeding from a G4-binding RGG peptide, 12, discovered above, we identified the cold-inducible RNA-binding protein (CIRBP) as a new G4 DNA-binding protein both in vitro and in cells. In addition, we found that the key amino acids for G4 binding in peptide 12 and CIRBP were highly similar, and peptide 12 clearly played a key role in the G4 binding of CIRBP. This report is the first in which a G4-binding protein was identified from exploration of the G4-binding RGG motif. Our findings suggest a novel strategy for discovering new G4-binding proteins by exploring key peptide segments.
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