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BAF 复合物因子 BRD9 的异双功能配体降解。

Degradation of the BAF Complex Factor BRD9 by Heterobifunctional Ligands.

机构信息

Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.

Department of Pediatric Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.

出版信息

Angew Chem Int Ed Engl. 2017 May 15;56(21):5738-5743. doi: 10.1002/anie.201611281. Epub 2017 Apr 18.

DOI:10.1002/anie.201611281
PMID:28418626
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5967236/
Abstract

The bromodomain-containing protein BRD9, a subunit of the human BAF (SWI/SNF) nucleosome remodeling complex, has emerged as an attractive therapeutic target in cancer. Despite the development of chemical probes targeting the BRD9 bromodomain, there is a limited understanding of BRD9 function beyond acetyl-lysine recognition. We have therefore created the first BRD9-directed chemical degraders, through iterative design and testing of heterobifunctional ligands that bridge the BRD9 bromodomain and the cereblon E3 ubiquitin ligase complex. Degraders of BRD9 exhibit markedly enhanced potency compared to parental ligands (10- to 100-fold). Parallel study of degraders with divergent BRD9-binding chemotypes in models of acute myeloid leukemia resolves bromodomain polypharmacology in this emerging drug class. Together, these findings reveal the tractability of non-BET bromodomain containing proteins to chemical degradation, and highlight lead compound dBRD9 as a tool for the study of BRD9.

摘要

溴结构域蛋白 BRD9 是人类 BAF(SWI/SNF)核小体重塑复合物的一个亚基,已成为癌症治疗的一个有吸引力的靶点。尽管已经开发出针对 BRD9 溴结构域的化学探针,但对 BRD9 功能的了解除了乙酰化赖氨酸识别之外还很有限。因此,我们通过反复设计和测试连接 BRD9 溴结构域和 cereblon E3 泛素连接酶复合物的杂双功能配体,创建了第一个 BRD9 定向化学降解剂。BRD9 的降解剂与亲本配体相比表现出明显增强的效力(10 到 100 倍)。在急性髓细胞白血病模型中对具有不同 BRD9 结合化学型的降解剂进行平行研究,解决了这个新兴药物类别中溴结构域多效性的问题。总之,这些发现表明非 BET 溴结构域蛋白对化学降解具有可操作性,并突出了先导化合物 dBRD9 作为研究 BRD9 的工具。

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