| Literature DB >> 32282883 |
Andrew S Moore1,2, Amir Faisal1, Grace W Y Mak1, Farideh Miraki-Moud1, Vassilios Bavetsias1, Melanie Valenti1, Gary Box1, Albert Hallsworth1, Alexis de Haven Brandon1, Cristina P R Xavier1, Randal Stronge1,3, Andrew D J Pearson1,2, Julian Blagg1, Florence I Raynaud1, Rajesh Chopra1, Suzanne A Eccles1, David C Taussig1,3, Spiros Linardopoulos1,4.
Abstract
Internal tandem duplication of FLT3 (FLT3-ITD) is one of the most common somatic mutations in acute myeloid leukemia (AML); it causes constitutive activation of FLT3 kinase and is associated with high relapse rates and poor survival. Small-molecule inhibition of FLT3 represents an attractive therapeutic strategy for this subtype of AML, although resistance from secondary FLT3 tyrosine kinase domain (FLT3-TKD) mutations is an emerging clinical problem. CCT241736 is an orally bioavailable, selective, and potent dual inhibitor of FLT3 and Aurora kinases. FLT3-ITD+ cells with secondary FLT3-TKD mutations have high in vitro relative resistance to the FLT3 inhibitors quizartinib and sorafenib, but not to CCT241736. The mechanism of action of CCT241736 results in significant in vivo efficacy, with inhibition of tumor growth observed in efficacy studies in FLT3-ITD and FLT3-ITD-TKD human tumor xenograft models. The efficacy of CCT241736 was also confirmed in primary samples from AML patients, including those with quizartinib-resistant disease, which induces apoptosis through inhibition of both FLT3 and Aurora kinases. The unique combination of CCT241736 properties based on robust potency, dual selectivity, and significant in vivo activity indicate that CCT241736 is a bona fide clinical drug candidate for FLT3-ITD and TKD AML patients with resistance to current drugs.Entities:
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Year: 2020 PMID: 32282883 PMCID: PMC7160287 DOI: 10.1182/bloodadvances.2019000986
Source DB: PubMed Journal: Blood Adv ISSN: 2473-9529