| Literature DB >> 24858910 |
Catherine Dehainault1, Alexandra Garancher2, Laurent Castéra1, Nathalie Cassoux3, Isabelle Aerts4, François Doz5, Laurence Desjardins6, Livia Lumbroso6, Rocío Montes de Oca7, Geneviève Almouzni7, Dominique Stoppa-Lyonnet8, Celio Pouponnot9, Marion Gauthier-Villars1, Claude Houdayer10.
Abstract
Retinoblastoma is a non-hereditary as well as an inherited pediatric tumor of the developing retina resulting from the inactivation of both copies of the RB1 tumor suppressor gene. Familial retinoblastoma is a highly penetrant genetic disease that usually develops by carrying germline mutations that inactivate one allele of the RB1 gene, leading to multiple retinoblastomas. However, large and complete germline RB1 deletions are associated with low or no tumor risk for reasons that remain unknown. In this study, we define a minimal genomic region associated with this low penetrance. This region encompasses few genes including MED4 a subunit of the mediator complex. We further show that retinoblastoma RB1 -/- cells cannot survive in the absence of MED4, both in vitro and in orthotopic xenograft models in vivo, therefore identifying MED4 as a survival gene in retinoblastoma. We propose that the contiguous loss of the adjacent retinoblastoma gene, MED4, explains the low penetrance in patients with large deletions that include both RB1 and MED4. Our findings also point to another synthetic lethal target in tumors with inactivated RB1 and highlight the importance of collateral damage in carcinogenesis.Entities:
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Year: 2014 PMID: 24858910 DOI: 10.1093/hmg/ddu245
Source DB: PubMed Journal: Hum Mol Genet ISSN: 0964-6906 Impact factor: 6.150