Discovery of a Small-Molecule Degrader of Bromodomain and Extra-Terminal (BET) Proteins with Picomolar Cellular Potencies and Capable of Achieving Tumor Regression

Bing Zhou; Jiantao Hu; Fuming Xu; Zhuo Chen; Longchuan Bai; Ester Fernandez-Salas; Mei Lin; Liu Liu; Chao-Yie Yang; Yujun Zhao; Donna McEachern; Sally Przybranowski; Bo Wen; Duxin Sun; Shaomeng Wang

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Discovery of a Small-Molecule Degrader of Bromodomain and Extra-Terminal (BET) Proteins with Picomolar Cellular Potencies and Capable of Achieving Tumor Regression

机译：发现菠萝蛋白酶和外末端（BET）蛋白的小分子降解剂，具有皮摩尔细胞效力，能够实现肿瘤回归

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The bromodomain and extra-terminal (BET) family proteins, consisting of BRD2, BRD3, BRD4, and testis-specific BRDT members, are epigenetic “readers” and play a key role in the regulation of gene transcription. BET proteins are considered to be attractive therapeutic targets for cancer and other human diseases. Recently, heterobifunctional small-molecule BET degraders have been designed based upon the proteolysis targeting chimera (PROTAC) concept to induce BET protein degradation. Herein, we present our design, synthesis, and evaluation of a new class of PROTAC BET degraders. One of the most promising compounds, 23 , effectively degrades BRD4 protein at concentrations as low as 30 pM in the RS4;11 leukemia cell line, achieves an IC_(50) value of 51 pM in inhibition of RS4;11 cell growth and induces rapid tumor regression in vivo against RS4;11 xenograft tumors. These data establish that compound 23 (BETd-260/ZBC260) is a highly potent and efficacious BET degrader.

机译：由BRD2，BRD3，BRD4和Testis特异性BRDT成员组成的溴琼瘤和终端（BET）家族蛋白质是表观遗传的“读者”，并在基因转录的调节中发挥关键作用。 BET蛋白被认为是有吸引力的癌症和其他人类疾病的治疗靶标。最近，基于靶向嵌合（Protac）概念的蛋白水解以诱导蛋白质降解的蛋白水解，设计了异质小分子BET降解剂。在此，我们展示了我们的设计，合成和评估新类Protac Bet降解剂。最有希望的化合物，23，在RS4中的浓度下有效地降解BRD4蛋白，在RS4; 11只白血病细胞系中达到低至30μm，抑制Rs4的抑制率为51μm的IC_（50）值; 11个细胞生长和诱导迅速体内肿瘤回归对抗Rs4; 11种异种移植肿瘤。这些数据建立了化合物23（BetD-260 / ZBC260）是一种高效且有效的下注剂。

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《Journal of Medicinal Chemistry 》 |2018年第2期| 共20页
作者
Bing Zhou; Jiantao Hu; Fuming Xu; Zhuo Chen; Longchuan Bai; Ester Fernandez-Salas; Mei Lin; Liu Liu; Chao-Yie Yang; Yujun Zhao; Donna McEachern; Sally Przybranowski; Bo Wen; Duxin Sun; Shaomeng Wang;
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University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

University of Michigan Comprehensive Cancer Center and Departments of Internal Medicine Pathology Pharmaceutical Sciences Medicinal Chemistry and Pharmacology University of Michigan Ann Arbor Michigan 48109 United States;

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1. Discovery of a Small-Molecule Degrader of Bromodomain and Extra-Terminal (BET) Proteins with Picomolar Cellular Potencies and Capable of Achieving Tumor Regression [J] . Bing Zhou, Jiantao Hu, Fuming Xu, Journal of Medicinal Chemistry . 2018 ,第2期

机译：发现菠萝蛋白酶和外末端（BET）蛋白的小分子降解剂，具有皮摩尔细胞效力，能够实现肿瘤回归
2. Discovery of QCA570 as an Exceptionally Potent and Efficacious Proteolysis Targeting Chimera (PROTAC) Degrader of the Bromodomain and Extra-Terminal (BET) Proteins Capable of Inducing Complete and Durable Tumor Regression [J] . Qin Chong, Hu Yang, Zhou Bing, Journal of Medicinal Chemistry . 2018 ,第15期

机译：发现QCA570作为靶向嵌合（Protac）靶向嵌合体（Protac）的靶向有效和有效的蛋白水溶性溴琼瘤和蛋白质（BET）蛋白质，其能够诱导完全和耐用的肿瘤回归
3. Discovery of novel small molecule induced selective degradation of the bromodomain and extra-terminal (BET) bromodomain protein BRD4 and BRD2 with cellular potencies [J] . Bioorganic and medicinal chemistry . 2020 ,第1期

机译：新型小分子的发现诱导了溴琼瘤和外末端（BET）溴蛋白BRD4和BRD2的选择性降解了细胞效力
4. INTERRELATIONSHIPS BETWEEN PROSTAGLANDINS, CYCLIC ADENOSINE 3',5'-MONOPHOSPHATE AND NUCLEAR PROTEIN PHOSPHORYLATION DURING INDUCED REGRESSION IN RAT MAMMARY TUMORS (CYCLIC-AMP). [D] . FOECKING, MARY KATHERINE. 1982

机译：大鼠乳腺肿瘤引起的衰老过程中前列腺素，循环腺嘌呤3'，5'-单磷酸盐和核蛋白磷酸化的相互关系。
5. Discovery of aSmall-Molecule Degrader of Bromodomainand Extra-Terminal (BET) Proteins with Picomolar Cellular Potenciesand Capable of Achieving Tumor Regression [O] . Bing Zhou, ∇, Jiantao Hu, -1

机译：发现一个溴结构域的小分子降解剂和末端（BET）蛋白具有皮摩尔细胞的潜能并且能够实现肿瘤消退
6. Discovery of QCA570 as an Exceptionally Potent and Efficacious Proteolysis Targeting Chimera (PROTAC) Degrader of the Bromodomain and Extra-Terminal (BET) Proteins Capable of Inducing Complete and Durable Tumor Regression [O] . Chong Qin, Yang Hu, Bing Zhou, 2018

机译：发现QCA570作为靶向嵌合（Protac）靶向嵌合体（Protac）的靶向有效和有效的蛋白水溶性溴琼瘤和蛋白质（BET）蛋白质，其能够诱导完全和耐用的肿瘤回归

Discovery of a Small-Molecule Degrader of Bromodomain and Extra-Terminal (BET) Proteins with Picomolar Cellular Potencies and Capable of Achieving Tumor Regression

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