KRAS Mouse Models: Modeling Cancer Harboring KRAS Mutations
- PMID: 21779503
- PMCID: PMC3128636
- DOI: 10.1177/1947601911408080
KRAS Mouse Models: Modeling Cancer Harboring KRAS Mutations
Abstract
KRAS is a potent oncogene and is mutated in about 30% of all human cancers. However, the biological context of KRAS-dependent oncogenesis is poorly understood. Genetically engineered mouse models of cancer provide invaluable tools to study the oncogenic process, and insights from KRAS-driven models have significantly increased our understanding of the genetic, cellular, and tissue contexts in which KRAS is competent for oncogenesis. Moreover, variation among tumors arising in mouse models can provide insight into the mechanisms underlying response or resistance to therapy in KRAS-dependent cancers. Hence, it is essential that models of KRAS-driven cancers accurately reflect the genetics of human tumors and recapitulate the complex tumor-stromal intercommunication that is manifest in human cancers. Here, we highlight the progress made in modeling KRAS-dependent cancers and the impact that these models have had on our understanding of cancer biology. In particular, the development of models that recapitulate the complex biology of human cancers enables translational insights into mechanisms of therapeutic intervention in KRAS-dependent cancers.
Keywords: interpatient tumor variation; mouse models harboring KRAS mutation; tumor context; tumor genetics.
Conflict of interest statement
The author(s) declared the following potential conflicts of interest with respect to the research, authorship, and/or publication of this article: Rónán O’Hagan and Joerg Heyer are full-time employees of AVEO Pharmaceuticals.
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