Widespread Selection for Oncogenic Mutant Allele Imbalance in Cancer.

Authors :: Bielski CM
Donoghue MTA
Gadiya M
Hanrahan AJ
Won HH
Chang MT
Jonsson P
Penson AV
Gorelick A
Harris C
Schram AM
Syed A
Zehir A
Chapman PB
Hyman DM
Solit DB
Shannon K
Chandarlapaty S
Berger MF
Taylor BS
Source :: Cancer cell [Cancer Cell] 2018 Nov 12; Vol. 34 (5), pp. 852-862.e4. Date of Electronic Publication: 2018 Nov 01.
Publication Year :: 2018
Abstract: Driver mutations in oncogenes encode proteins with gain-of-function properties that enhance fitness. Heterozygous mutations are thus viewed as sufficient for tumorigenesis. We describe widespread oncogenic mutant allele imbalance in 13,448 prospectively characterized cancers. Imbalance was selected for through modest dosage increases of gain-of-fitness mutations. Negative selection targeted haplo-essential effectors of the spliceosome. Loss of the normal allele comprised a distinct class of imbalance driven by competitive fitness, which correlated with enhanced response to targeted therapies. In many cancers, an antecedent oncogenic mutation drove evolutionarily dependent allele-specific imbalance. In other instances, oncogenic mutations co-opted independent copy-number changes via the evolutionary process of exaptation. Oncogenic allele imbalance is a pervasive evolutionary innovation that enhances fitness and modulates sensitivity to targeted therapy.<br /> (Copyright © 2018 Elsevier Inc. All rights reserved.)