Promoterless Transposon Mutagenesis Drives Solid Cancers via Tumor Suppressor Inactivation

Author:

Aiderus AzizORCID,Contreras-Sandoval Ana M.ORCID,Meshey Amanda L.,Newberg Justin Y.,Ward Jerrold M.,Swing Deborah A.,Copeland Neal G.,Jenkins Nancy A.,Mann Karen M.ORCID,Mann Michael B.ORCID

Abstract

A central challenge in cancer genomics is the systematic identification of single and cooperating tumor suppressor gene mutations driving cellular transformation and tumor progression in the absence of oncogenic driver mutation(s). Multiple in vitro and in vivo gene inactivation screens have enhanced our understanding of the tumor suppressor gene landscape in various cancers. However, these studies are limited to single or combination gene effects, specific organs, or require sensitizing mutations. In this study, we developed and utilized a Sleeping Beauty transposon mutagenesis system that functions only as a gene trap to exclusively inactivate tumor suppressor genes. Using whole body transposon mobilization in wild type mice, we observed that cumulative gene inactivation can drive tumorigenesis of solid cancers. We provide a quantitative landscape of the tumor suppressor genes inactivated in these cancers and show that, despite the absence of oncogenic drivers, these genes converge on key biological pathways and processes associated with cancer hallmarks.

Funder

H. Lee Moffitt Cancer Center and Research Institute

Cancer Prevention and Research Institute of Texas

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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