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Literature DB >> 15744054

Synthetic lethality of retinoblastoma mutant cells in the Drosophila eye by mutation of a novel peptidyl prolyl isomerase gene.

Kyle A Edgar¹, Marcia Belvin, Annette L Parks, Kellie Whittaker, Matt B Mahoney, Monique Nicoll, Christopher C Park, Christopher G Winter, Feng Chen, Kim Lickteig, Ferhad Ahmad, Hanife Esengil, Matthew V Lorenzi, Amanda Norton, Brent A Rupnow, Laleh Shayesteh, Mariano Tabios, Lynn M Young, Pamela M Carroll, Casey Kopczynski, Gregory D Plowman, Lori S Friedman, Helen L Francis-Lang.

Abstract

Mutations that inactivate the retinoblastoma (Rb) pathway are common in human tumors. Such mutations promote tumor growth by deregulating the G1 cell cycle checkpoint. However, uncontrolled cell cycle progression can also produce new liabilities for cell survival. To uncover such liabilities in Rb mutant cells, we performed a clonal screen in the Drosophila eye to identify second-site mutations that eliminate Rbf(-) cells, but allow Rbf(+) cells to survive. Here we report the identification of a mutation in a novel highly conserved peptidyl prolyl isomerase (PPIase) that selectively eliminates Rbf(-) cells from the Drosophila eye.

Entities: Disease Gene Species

Mesh：

Substances：

Year: 2005 PMID： 15744054 PMCID： PMC1449713 DOI： 10.1534/genetics.104.036343

Source DB: PubMed Journal: Genetics ISSN： 0016-6731 Impact factor: 4.562

38 in total

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