Literature DB >> 21746896

Systematic investigation of genetic vulnerabilities across cancer cell lines reveals lineage-specific dependencies in ovarian cancer.

Hiu Wing Cheung1, Glenn S Cowley, Barbara A Weir, Jesse S Boehm, Scott Rusin, Justine A Scott, Alexandra East, Levi D Ali, Patrick H Lizotte, Terence C Wong, Guozhi Jiang, Jessica Hsiao, Craig H Mermel, Gad Getz, Jordi Barretina, Shuba Gopal, Pablo Tamayo, Joshua Gould, Aviad Tsherniak, Nicolas Stransky, Biao Luo, Yin Ren, Ronny Drapkin, Sangeeta N Bhatia, Jill P Mesirov, Levi A Garraway, Matthew Meyerson, Eric S Lander, David E Root, William C Hahn.   

Abstract

A comprehensive understanding of the molecular vulnerabilities of every type of cancer will provide a powerful roadmap to guide therapeutic approaches. Efforts such as The Cancer Genome Atlas Project will identify genes with aberrant copy number, sequence, or expression in various cancer types, providing a survey of the genes that may have a causal role in cancer. A complementary approach is to perform systematic loss-of-function studies to identify essential genes in particular cancer cell types. We have begun a systematic effort, termed Project Achilles, aimed at identifying genetic vulnerabilities across large numbers of cancer cell lines. Here, we report the assessment of the essentiality of 11,194 genes in 102 human cancer cell lines. We show that the integration of these functional data with information derived from surveying cancer genomes pinpoints known and previously undescribed lineage-specific dependencies across a wide spectrum of cancers. In particular, we found 54 genes that are specifically essential for the proliferation and viability of ovarian cancer cells and also amplified in primary tumors or differentially overexpressed in ovarian cancer cell lines. One such gene, PAX8, is focally amplified in 16% of high-grade serous ovarian cancers and expressed at higher levels in ovarian tumors. Suppression of PAX8 selectively induces apoptotic cell death of ovarian cancer cells. These results identify PAX8 as an ovarian lineage-specific dependency. More generally, these observations demonstrate that the integration of genome-scale functional and structural studies provides an efficient path to identify dependencies of specific cancer types on particular genes and pathways.

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Year:  2011        PMID: 21746896      PMCID: PMC3145679          DOI: 10.1073/pnas.1109363108

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  28 in total

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Journal:  Nature       Date:  2005-07-07       Impact factor: 49.962

4.  Emerging roles for PAX8 in ovarian cancer and endosalpingeal development.

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9.  Integrated genomic analyses of ovarian carcinoma.

Authors: 
Journal:  Nature       Date:  2011-06-29       Impact factor: 49.962

Review 10.  Pax genes in embryogenesis and oncogenesis.

Authors:  Qiuyu Wang; Wen-Hui Fang; Jerzy Krupinski; Shant Kumar; Mark Slevin; Patricia Kumar
Journal:  J Cell Mol Med       Date:  2008-07-04       Impact factor: 5.310

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  237 in total

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2.  The Tyrosine Kinase Adaptor Protein FRS2 Is Oncogenic and Amplified in High-Grade Serous Ovarian Cancer.

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3.  CD133 protein N-glycosylation processing contributes to cell surface recognition of the primitive cell marker AC133 epitope.

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4.  ScreenBEAM: a novel meta-analysis algorithm for functional genomics screens via Bayesian hierarchical modeling.

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5.  Collateral Lethality: A new therapeutic strategy in oncology.

Authors:  Florian L Muller; Elisa A Aquilanti; Ronald A DePinho
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7.  Comprehensive Mapping of Pluripotent Stem Cell Metabolism Using Dynamic Genome-Scale Network Modeling.

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Review 8.  Fallopian tube initiation of high grade serous ovarian cancer and ovarian metastasis: Mechanisms and therapeutic implications.

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9.  Synthetic lethality between CCNE1 amplification and loss of BRCA1.

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10.  The EMT regulator ZEB2 is a novel dependency of human and murine acute myeloid leukemia.

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