| Literature DB >> 28215705 |
Michael R Burgess1, Eugene Hwang2, Rana Mroue3, Craig M Bielski4, Anica M Wandler2, Benjamin J Huang2, Ari J Firestone2, Amy Young5, Jennifer A Lacap5, Lisa Crocker5, Saurabh Asthana1, Elizabeth M Davis6, Jin Xu2, Keiko Akagi7, Michelle M Le Beau6, Qing Li8, Benjamin Haley9, David Stokoe3, Deepak Sampath5, Barry S Taylor10, Marie Evangelista11, Kevin Shannon12.
Abstract
Investigating therapeutic "outliers" that show exceptional responses to anti-cancer treatment can uncover biomarkers of drug sensitivity. We performed preclinical trials investigating primary murine acute myeloid leukemias (AMLs) generated by retroviral insertional mutagenesis in KrasG12D "knockin" mice with the MEK inhibitor PD0325901 (PD901). One outlier AML responded and exhibited intrinsic drug resistance at relapse. Loss of wild-type (WT) Kras enhanced the fitness of the dominant clone and rendered it sensitive to MEK inhibition. Similarly, human colorectal cancer cell lines with increased KRAS mutant allele frequency were more sensitive to MAP kinase inhibition, and CRISPR-Cas9-mediated replacement of WT KRAS with a mutant allele sensitized heterozygous mutant HCT116 cells to treatment. In a prospectively characterized cohort of patients with advanced cancer, 642 of 1,168 (55%) with KRAS mutations exhibited allelic imbalance. These studies demonstrate that serial genetic changes at the Kras/KRAS locus are frequent in cancer and modulate competitive fitness and MEK dependency.Entities:
Keywords: AML; KRAS; MEK inhibition; allelic imbalance; colorectal cancer; drug resistance
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Year: 2017 PMID: 28215705 PMCID: PMC5541948 DOI: 10.1016/j.cell.2017.01.020
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582