Paralogue-Selective Degradation of the Lysine Acetyltransferase EP300

JACS Au Pub Date : 2024-07-29 DOI:10.1021/jacsau.4c00442

Xuemin Chen, McKenna C. Crawford, Ying Xiong, Anver Basha Shaik, Kiall F. Suazo, Ludwig G. Bauer, Manini S. Penikalapati, Joycelyn H. Williams, Kilian V. M. Huber, Thorkell Andressen, Rolf E. Swenson, Jordan L. Meier

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Abstract

The transcriptional coactivators EP300 and CREBBP are critical regulators of gene expression that share high sequence identity but exhibit nonredundant functions in basal and pathological contexts. Here, we report the development of a bifunctional small molecule, MC-1, capable of selectively degrading EP300 over CREBBP. Using a potent aminopyridine-based inhibitor of the EP300/CREBBP catalytic domain in combination with a VHL ligand, we demonstrate that MC-1 preferentially degrades EP300 in a proteasome-dependent manner. Mechanistic studies reveal that selective degradation cannot be predicted solely by target engagement or ternary complex formation, suggesting additional factors govern paralogue-specific degradation. MC-1 inhibits cell proliferation in a subset of cancer cell lines and provides a new tool to investigate the noncatalytic functions of EP300 and CREBBP. Our findings expand the repertoire of EP300/CREBBP-targeting chemical probes and offer insights into the determinants of selective degradation of highly homologous proteins.

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赖氨酸乙酰转移酶 EP300 的旁系选择性降解

转录辅激活因子 EP300 和 CREBBP 是基因表达的关键调控因子，它们具有高度的序列同一性，但在基础和病理环境中表现出非冗余的功能。在这里，我们报告了一种双功能小分子 MC-1 的开发情况，它能够选择性地降解 EP300 而不是 CREBBP。利用一种基于氨基吡啶的 EP300/CREBBP 催化结构域强效抑制剂与 VHL 配体的结合，我们证明 MC-1 能以蛋白酶体依赖的方式优先降解 EP300。机理研究显示，选择性降解不能仅通过靶标参与或三元复合物形成来预测，这表明还有其他因素在支配着副对映体特异性降解。MC-1 能抑制一部分癌细胞系的细胞增殖，为研究 EP300 和 CREBBP 的非催化功能提供了一种新工具。我们的研究结果扩大了 EP300/CREBBP 靶向化学探针的范围，并为高度同源蛋白选择性降解的决定因素提供了见解。

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