Discovery of WEE1 Kinase Inhibitors with Potent Activity against Patient-Derived, Metastatic Colorectal Cancer Organoids

IF 6.8 1区医学 Q1 CHEMISTRY, MEDICINAL Journal of Medicinal Chemistry Pub Date : 2025-04-10 DOI:10.1021/acs.jmedchem.4c02541

Joel L. Syphers, Josephine A. Wright, Shen Liu, Yi Sing Gee, Fan Gao, Ramesh Mudududdla, Da Qing Che, Aeson Chang, Erica K. Sloan, Vignesh Narasimhan, Alexander Heriot, Robert G. Ramsay, Rebekah de Nys, Tharindie N. Silva, Laura Vrbanac, Tarik Sammour, Matthew J. Lawrence, Teresa Tin, Guy J. Maddern, Kevin Fenix, Harleen Kaur, Kate Barratt, Gerhard Kelter, Armin Maier, Markus Posch, Hongfu Lu, Xiaomin Wang, Alex Zhavoronkov, Heping Wei, Fei Huang, Daniel L. Worthley, Daniel L. Priebbenow, Siddhartha Mukherjee, Susan L. Woods, Jonathan B. Baell

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Abstract

A library of potent WEE1 kinase inhibitors was synthesized based on the discontinued frontrunner clinical candidate AZD1775 (1), many of which were more selective for WEE1 over an undesirable off-target of 1, the kinase PLK1. When tested against patient-derived organoids (PDOs) grown from TP53-mutated colorectal cancer (CRC) peritoneal metastases, 34 (IC₅₀ value of 62 nM) exhibited stronger efficacy than 1 (IC₅₀ value of 120 nM) and the best-in-class clinical candidate ZN-c3 (IC₅₀ value of 127 nM). Against primary CRC PDOs with TP53-WT, 34 significantly enhanced DNA damage, replication stress and apoptosis compared to 1, as well as demonstrated high selectivity over patient-matched normal healthy colon PDOs, highlighting a potential therapeutic window for cancer treatment. Overall, this investigation provides critical insight into several potent WEE1 inhibitors that exhibited exceptional efficacy against CRC PDOs and is the first to utilize a PDO platform to assess their effect on healthy and malignant cell viability.

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WEE1激酶抑制剂对患者来源的转移性结直肠癌类器官具有有效活性的发现

基于已停用的临床候选药物AZD1775(1)，我们合成了一个有效的WEE1激酶抑制剂库，其中许多抑制剂对WEE1具有更强的选择性，而不是对1的不良脱靶激酶PLK1。当对从tp53突变的结直肠癌（CRC）腹膜转移瘤中生长的患者源性类器官（PDOs）进行测试时，34 （IC50值为62 nM）表现出比1 （IC50值为120 nM）和同类最佳临床候选者ZN-c3 （IC50值为127 nM）更强的疗效。对于携带TP53-WT的原发性结直肠癌PDOs，与1相比，34显著增强了DNA损伤、复制应激和凋亡，并且对患者匹配的正常健康结肠PDOs表现出高选择性，突出了癌症治疗的潜在治疗窗口。总的来说，这项研究为几种有效的WEE1抑制剂提供了重要的见解，这些抑制剂对CRC PDO表现出卓越的疗效，并且是第一次利用PDO平台评估它们对健康和恶性细胞活力的影响。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Medicinal Chemistry 医学-医药化学

CiteScore

4.00

自引率

11.00%

发文量

804

审稿时长

1.9 months

期刊介绍： The Journal of Medicinal Chemistry is a prestigious biweekly peer-reviewed publication that focuses on the multifaceted field of medicinal chemistry. Since its inception in 1959 as the Journal of Medicinal and Pharmaceutical Chemistry, it has evolved to become a cornerstone in the dissemination of research findings related to the design, synthesis, and development of therapeutic agents. The Journal of Medicinal Chemistry is recognized for its significant impact in the scientific community, as evidenced by its 2022 impact factor of 7.3. This metric reflects the journal's influence and the importance of its content in shaping the future of drug discovery and development. The journal serves as a vital resource for chemists, pharmacologists, and other researchers interested in the molecular mechanisms of drug action and the optimization of therapeutic compounds.