| Literature DB >> 26202014 |
Mark D Gurden1, Isaac M Westwood2, Amir Faisal3, Sébastien Naud3, Kwai-Ming J Cheung3, Craig McAndrew3, Amy Wood3, Jessica Schmitt3, Kathy Boxall3, Grace Mak3, Paul Workman3, Rosemary Burke3, Swen Hoelder3, Julian Blagg3, Rob L M Van Montfort2, Spiros Linardopoulos4.
Abstract
Acquired resistance to therapy is perhaps the greatest challenge to effective clinical management of cancer. With several inhibitors of the mitotic checkpoint kinase MPS1 in preclinical development, we sought to investigate how resistance against these inhibitors may arise so that mitigation or bypass strategies could be addressed as early as possible. Toward this end, we modeled acquired resistance to the MPS1 inhibitors AZ3146, NMS-P715, and CCT251455, identifying five point mutations in the kinase domain of MPS1 that confer resistance against multiple inhibitors. Structural studies showed how the MPS1 mutants conferred resistance by causing steric hindrance to inhibitor binding. Notably, we show that these mutations occur in nontreated cancer cell lines and primary tumor specimens, and that they also preexist in normal lymphoblast and breast tissues. In a parallel piece of work, we also show that the EGFR p.T790M mutation, the most common mutation conferring resistance to the EGFR inhibitor gefitinib, also preexists in cancer cells and normal tissue. Our results therefore suggest that mutations conferring resistance to targeted therapy occur naturally in normal and malignant cells and these mutations do not arise as a result of the increased mutagenic plasticity of cancer cells. ©2015 American Association for Cancer Research.Entities:
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Year: 2015 PMID: 26202014 DOI: 10.1158/0008-5472.CAN-14-3272
Source DB: PubMed Journal: Cancer Res ISSN: 0008-5472 Impact factor: 12.701