Early TP53 alterations engage environmental exposures to promote gastric premalignancy in an integrative mouse model Journal Article


Authors: Sethi, N. S.; Kikuchi, O.; Duronio, G. N.; Stachler, M. D.; McFarland, J. M.; Ferrer-Luna, R.; Zhang, Y.; Bao, C.; Bronson, R.; Patil, D.; Sanchez-Vega, F.; Liu, J. B.; Sicinska, E.; Lazaro, J. B.; Ligon, K. L.; Beroukhim, R.; Bass, A. J.
Article Title: Early TP53 alterations engage environmental exposures to promote gastric premalignancy in an integrative mouse model
Abstract: Somatic alterations in cancer genes are being detected in normal and premalignant tissue, thus placing greater emphasis on gene–environment interactions that enable disease phenotypes. By combining early genetic alterations with disease-relevant exposures, we developed an integrative mouse model to study gastric premalignancy. Deletion of Trp53 in gastric cells confers a selective advantage and promotes the development of dysplasia in the setting of dietary carcinogens. Organoid derivation from dysplastic lesions facilitated genomic, transcriptional and functional evaluation of gastric premalignancy. Cell cycle regulators, most notably Cdkn2a, were upregulated by p53 inactivation in gastric premalignancy, serving as a barrier to disease progression. Co-deletion of Cdkn2a and Trp53 in dysplastic gastric organoids promoted cancer phenotypes but also induced replication stress, exposing a susceptibility to DNA damage response inhibitors. These findings demonstrate the utility of mouse models that integrate genomic alterations with relevant exposures and highlight the importance of gene–environment interactions in shaping the premalignant state. © 2020, The Author(s), under exclusive licence to Springer Nature America, Inc.
Journal Title: Nature Genetics
Volume: 52
Issue: 2
ISSN: 1061-4036
Publisher: Nature Publishing Group  
Date Published: 2020-02-01
Start Page: 219
End Page: 230
Language: English
DOI: 10.1038/s41588-019-0574-9
PUBMED: 32025000
PROVIDER: scopus
PMCID: PMC7031028
DOI/URL:
Notes: Article -- Export Date: 1 April 2020 -- Source: Scopus
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