核糖体 H2A K13/15 单泛素化和 RNF168 邻近双重单泛素化的机制

IF 12.9 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Huasong Ai, Zebin Tong, Zhiheng Deng, Qiang Shi, Shixian Tao, Gaoge Sun, Jiawei Liang, Maoshen Sun, Xiangwei Wu, Qingyun Zheng, Lujun Liang, Hang Yin, Jia-Bin Li, Shuai Gao, Changlin Tian, Lei Liu, Man Pan
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引用次数: 0

摘要

DNA损伤修复调控蛋白RNF168是一种单体RING型E3连接酶,通过特异性地、高效地泛素化H2A N端尾部相邻的K13和K15(K13/15)位点,在调控细胞命运和DNA修复方面发挥着至关重要的作用。然而,长期以来,由于缺乏 RNF168 和 UbcH5c~Ub (泛素)与核小体复合物的高分辨率结构,人们一直无法了解 RNF168 如何与其同源的 E2 酶 UbcH5c 相互配合,从而特异性地泛素化 H2A K13/15。在这里,我们开发了化学策略,并确定了在瞬时 H2A K13/15 单泛素化和相邻双单泛素化反应中捕获的 RNF168-UbcH5c~Ub 核小体复合物的冷冻电镜结构,提供了单体 E3 连接酶 RNF168 在核小体上的 "螺旋锚定 "模式,与二聚体 E3 连接酶的 "罗盘结合 "模式形成对比。我们的研究不仅提供了 H2A K13/15 位点特异性单泛素化和相邻双单泛素化的结构快照,还为理解 RNF168 的致病氨基酸取代和生理修饰提供了近乎原子分辨率的结构框架。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Mechanism of nucleosomal H2A K13/15 monoubiquitination and adjacent dual monoubiquitination by RNF168

Mechanism of nucleosomal H2A K13/15 monoubiquitination and adjacent dual monoubiquitination by RNF168

The DNA damage repair regulatory protein RNF168, a monomeric RING-type E3 ligase, has a crucial role in regulating cell fate and DNA repair by specific and efficient ubiquitination of the adjacent K13 and K15 (K13/15) sites at the H2A N-terminal tail. However, understanding how RNF168 coordinates with its cognate E2 enzyme UbcH5c to site-specifically ubiquitinate H2A K13/15 has long been hampered by the lack of high-resolution structures of RNF168 and UbcH5c~Ub (ubiquitin) in complex with nucleosomes. Here we developed chemical strategies and determined the cryo-electron microscopy structures of the RNF168–UbcH5c~Ub–nucleosome complex captured in transient H2A K13/15 monoubiquitination and adjacent dual monoubiquitination reactions, providing a ‘helix-anchoring’ mode for monomeric E3 ligase RNF168 on nucleosome in contrast to the ‘compass-binding’ mode of dimeric E3 ligases. Our work not only provides structural snapshots of H2A K13/15 site-specific monoubiquitination and adjacent dual monoubiquitination but also offers a near-atomic-resolution structural framework for understanding pathogenic amino acid substitutions and physiological modifications of RNF168.

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来源期刊
Nature chemical biology
Nature chemical biology 生物-生化与分子生物学
CiteScore
23.90
自引率
1.40%
发文量
238
审稿时长
12 months
期刊介绍: Nature Chemical Biology stands as an esteemed international monthly journal, offering a prominent platform for the chemical biology community to showcase top-tier original research and commentary. Operating at the crossroads of chemistry, biology, and related disciplines, chemical biology utilizes scientific ideas and approaches to comprehend and manipulate biological systems with molecular precision. The journal embraces contributions from the growing community of chemical biologists, encompassing insights from chemists applying principles and tools to biological inquiries and biologists striving to comprehend and control molecular-level biological processes. We prioritize studies unveiling significant conceptual or practical advancements in areas where chemistry and biology intersect, emphasizing basic research, especially those reporting novel chemical or biological tools and offering profound molecular-level insights into underlying biological mechanisms. Nature Chemical Biology also welcomes manuscripts describing applied molecular studies at the chemistry-biology interface due to the broad utility of chemical biology approaches in manipulating or engineering biological systems. Irrespective of scientific focus, we actively seek submissions that creatively blend chemistry and biology, particularly those providing substantial conceptual or methodological breakthroughs with the potential to open innovative research avenues. The journal maintains a robust and impartial review process, emphasizing thorough chemical and biological characterization.
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