Design Synthesis and Biological Activity of 123-TriazolobenzodiazepineBET Bromodomain Inhibitors

机译：123-三唑并苯并二氮杂pine的设计合成及生物活性BET溴结构域抑制剂

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A number of diazepines are known to inhibit bromo- and extra-terminal domain (BET) proteins. Their BET inhibitory activity derives from the fusion of an acetyl-lysine mimetic heterocycle onto the diazepine framework. Herein we describe a straightforward, modular synthesis of novel 1,2,3-triazolobenzodiazepines and show that the 1,2,3-triazole acts as an effective acetyl-lysine mimetic heterocycle. Structure-based optimization of this series of compounds led to the development of potent BET bromodomain inhibitors with excellent activity against leukemic cells, concomitant with a reduction in c-MYC expression. These novel benzodiazepines therefore represent a promising class of therapeutic BET inhibitors.

机译：已知许多二氮杂卓可抑制溴末端和末端外域（BET）蛋白。它们的BET抑制活性源自乙酰赖氨酸模拟杂环在二氮杂骨架上的融合。在这里，我们描述了新颖的1,2,3-三唑并苯并二氮杂a的简单，模块化合成，并表明1,2,3-三唑可作为有效的乙酰赖氨酸模拟杂环。该系列化合物的基于结构的优化导致开发出有效的BET溴结构域抑制剂，该抑制剂对白血病细胞具有出色的活性，并伴随c-MYC表达的降低。因此，这些新颖的苯二氮卓类代表了有前途的治疗性BET抑制剂。

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期刊名称 ACS Medicinal Chemistry Letters
作者
PhillipP. Sharp; □; ◆; Jean-Marc Garnier; ◆; Tamas Hatfaludi; ◆; Zhen Xu; David Segal; Kate E. Jarman; Hélène Jousset; Alexandra Garnham; John T. Feutrill; Anthony Cuzzupe; Peter Hall; Scott Taylor; Carl R. Walkley; Dean Tyler; Mark A. Dawson; Peter Czabotar; Andrew F. Wilks; Stefan Glaser; David C. S. Huang; Christopher J. Burns; *;
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年(卷),期 2017(8),12
年度 2017
页码 1298–1303
总页数 6
原文格式 PDF
正文语种
中图分类药物化学;
关键词
Bromodomain JQ1 triazole leukemia benzodiazepine;

机译：溴结构域;JQ1;三唑;白血病;苯二氮卓;

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1. Design, Synthesis, and Biological Activity of 1,2,3-Triazolobenzodiazepine BET Bromodomain Inhibitors [J] . Phillip P. Sharp, Jean-Marc Garnier, Tamas Hatfaludi, ACS medicinal chemistry letters . 2017,第12期

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5. Design and synthesis of core structural intermediates for novel HIV-1 protease inhibitors and synthesis, biological activity and molecular modeling of novel 20S proteasome inhibitors. [D] . Avancha, Kiran Kumar Venkata Raja. 2006

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6. A New CDK2 Inhibitor with 3-Hydrazonoindolin-2-One Scaffold Endowed with Anti-Breast Cancer Activity: Design Synthesis Biological Evaluation and In Silico Insights [O] . Mohammad M. Al-Sanea, Ahmad J. Obaidullah, Mohamed E. Shaker, 2021

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Design Synthesis and Biological Activity of 123-TriazolobenzodiazepineBET Bromodomain Inhibitors

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