Title of article
A Genome-wide RNAi Screen Identifies Multiple Synthetic Lethal Interactions with the Ras Oncogene
Author/Authors
Ji Luo، نويسنده , , Michael J. Emanuele، نويسنده , , Danan Li، نويسنده , , Chad J. Creighton، نويسنده , , Michael R. Schlabach، نويسنده , , Thomas F. Westbrook، نويسنده , , Kwok-Kin Wong، نويسنده , , Stephen J. Elledge، نويسنده ,
Issue Information
هفته نامه با شماره پیاپی سال 2009
Pages
14
From page
835
To page
848
Abstract
Oncogenic mutations in the small GTPase Ras are highly prevalent in cancer, but an understanding of the vulnerabilities of these cancers is lacking. We undertook a genome-wide RNAi screen to identify synthetic lethal interactions with the KRAS oncogene. We discovered a diverse set of proteins whose depletion selectively impaired the viability of Ras mutant cells. Among these we observed a strong enrichment for genes with mitotic functions. We describe a pathway involving the mitotic kinase PLK1, the anaphase-promoting complex/cyclosome, and the proteasome that, when inhibited, results in prometaphase accumulation and the subsequent death of Ras mutant cells. Gene expression analysis indicates that reduced expression of genes in this pathway correlates with increased survival of patients bearing tumors with a Ras transcriptional signature. Our results suggest a previously underappreciated role for Ras in mitotic progression and demonstrate a pharmacologically tractable pathway for the potential treatment of cancers harboring Ras mutations.
Journal title
CELL
Serial Year
2009
Journal title
CELL
Record number
1019767
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