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多功能合成核小体的开发,以探究染色质介导的蛋白质相互作用。

Development of multifunctional synthetic nucleosomes to interrogate chromatin-mediated protein interactions.

机构信息

Department of Chemistry, The University of Hong Kong, Pokfulam, Hong Kong, China.

Greater Bay Biomedical InnoCenter, Shenzhen Bay Laboratory (SZBL), Shenzhen 518055, China.

出版信息

Sci Adv. 2023 May 3;9(18):eade5186. doi: 10.1126/sciadv.ade5186.

Abstract

Various proteins bind to chromatin to regulate DNA and its associated processes such as replication, transcription, and damage repair. The identification and characterization of these chromatin-associating proteins remain a challenge, as their interactions with chromatin often occur within the context of the local nucleosome or chromatin structure, which makes conventional peptide-based strategies unsuitable. Here, we developed a simple and robust protein labeling chemistry to prepare synthetic multifunctional nucleosomes that carry a photoreactive group, a biorthogonal handle, and a disulfide moiety to examine chromatin-protein interactions in a nucleosomal context. Using the prepared protein- and nucleosome-based photoaffinity probes, we examined a number of protein-protein and protein-nucleosome interactions. In particular, we (i) mapped the binding sites for the HMGN2-nucleosome interaction, (ii) provided the evidence for transition between the active and poised states of DOT1L in recognizing H3K79 within the nucleosome, and (iii) identified OARD1 and LAP2α as nucleosome acidic patch-associating proteins. This study provides powerful and versatile chemical tools for interrogating chromatin-associating proteins.

摘要

各种蛋白质与染色质结合,以调节 DNA 及其相关过程,如复制、转录和损伤修复。鉴定和表征这些与染色质结合的蛋白质仍然是一个挑战,因为它们与染色质的相互作用通常发生在局部核小体或染色质结构的背景下,这使得传统的基于肽的策略不适用。在这里,我们开发了一种简单而强大的蛋白质标记化学方法,以制备携带光反应基团、生物正交接头和二硫键部分的合成多功能核小体,以在核小体环境中研究染色质-蛋白质相互作用。使用制备的基于蛋白质和核小体的光亲和探针,我们研究了许多蛋白质-蛋白质和蛋白质-核小体相互作用。特别是,我们 (i) 绘制了 HMGN2-核小体相互作用的结合位点,(ii) 提供了证据证明 DOT1L 在核小体中识别 H3K79 时从活性状态到静止状态的转变,以及 (iii) 鉴定了 OARD1 和 LAP2α 作为核小体酸性斑结合蛋白。这项研究为研究与染色质结合的蛋白质提供了强大而通用的化学工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3de6/10156118/bfeb15075c2e/sciadv.ade5186-f1.jpg

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