| Literature DB >> 29683659 |
Kurt G Pike1, Bernard Barlaam1, Elaine Cadogan1, Andrew Campbell2, Yingxue Chen3, Nicola Colclough1, Nichola L Davies1, Camila de-Almeida1, Sebastien L Degorce1,4, Myriam Didelot4, Allan Dishington5, Richard Ducray4, Stephen T Durant1, Lorraine A Hassall5, Jane Holmes5, Gareth D Hughes1, Philip A MacFaul5, Keith R Mulholland6, Thomas M McGuire1, Gilles Ouvry4, Martin Pass1, Graeme Robb1, Natalie Stratton7, Zhenhua Wang8, Joanne Wilson1, Baochang Zhai8, Kang Zhao8, Nidal Al-Huniti3.
Abstract
ATM inhibitors, such as 7, have demonstrated the antitumor potential of ATM inhibition when combined with DNA double-strand break-inducing agents in mouse xenograft models. However, the properties of 7 result in a relatively high predicted clinically efficacious dose. In an attempt to minimize attrition during clinical development, we sought to identify ATM inhibitors with a low predicted clinical dose (<50 mg) and focused on strategies to increase both ATM potency and predicted human pharmacokinetic half-life (predominantly through the increase of volume of distribution). These efforts resulted in the discovery of 64 (AZD0156), an exceptionally potent and selective inhibitor of ATM based on an imidazo[4,5- c]quinolin-2-one core. 64 has good preclinical phamacokinetics, a low predicted clinical dose, and a high maximum absorbable dose. 64 has been shown to potentiate the efficacy of the approved drugs irinotecan and olaparib in disease relevant mouse models and is currently undergoing clinical evaluation with these agents.Entities:
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Year: 2018 PMID: 29683659 DOI: 10.1021/acs.jmedchem.7b01896
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446