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

JL Syphers; JA Wright; S Liu; YS Gee; F Gao; R Mudududdla; DQ Che; A Chang; EK Sloan; V Narasimhan; A Heriot; RG Ramsay; R de Nys; TN Silva; L Vrbanac; T Sammour; MJ Lawrence; T Tin; GJ Maddern; K Fenix; H Kaur; K Barratt; G Kelter; A Maier; M Posch; H Lu; X Wang; A Zhavoronkov; H Wei; F Huang; DL Worthley; DL Priebbenow; S Mukherjee; SL Woods; JB Baell

Journal article

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

JL Syphers, JA Wright, S Liu, YS Gee, F Gao, R Mudududdla, DQ Che, A Chang, EK Sloan, V Narasimhan, A Heriot, RG Ramsay, R de Nys, TN Silva, L Vrbanac, T Sammour, MJ Lawrence, T Tin, GJ Maddern, K Fenix Show all

Journal of Medicinal Chemistry | Published : 2025

DOI: 10.1021/acs.jmedchem.4c02541

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 he..

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