Synthetic lethal screen identification of chemosensitizer loci in cancer cells

Angelique W Whitehurst; Brian O Bodemann; Jessica Cardenas; Deborah Ferguson; Luc Girard; Michael Peyton; John D Minna; Carolyn Michnoff; Weihua Hao; Michael G Roth; Xian-Jin Xie; Michael A White

doi:10.1038/nature05697

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Synthetic lethal screen identification of chemosensitizer loci in cancer cells

Journal article

Peer reviewed

Synthetic lethal screen identification of chemosensitizer loci in cancer cells

Angelique W Whitehurst, Brian O Bodemann, Jessica Cardenas, Deborah Ferguson, Luc Girard, Michael Peyton, John D Minna, Carolyn Michnoff, Weihua Hao, Michael G Roth, …

Nature (London), Vol.446(7137), pp.815-819

04/12/2007

DOI: 10.1038/nature05697

PMID: 17429401

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Abstract

Abundant evidence suggests that a unifying principle governing the molecular pathology of cancer is the co-dependent aberrant regulation of core machinery driving proliferation and suppressing apoptosis. Anomalous proteins engaged in support of this tumorigenic regulatory environment most probably represent optimal intervention targets in a heterogeneous population of cancer cells. The advent of RNA-mediated interference (RNAi)-based functional genomics provides the opportunity to derive unbiased comprehensive collections of validated gene targets supporting critical biological systems outside the framework of preconceived notions of mechanistic relationships. We have combined a high-throughput cell-based one-well/one-gene screening platform with a genome-wide synthetic library of chemically synthesized small interfering RNAs for systematic interrogation of the molecular underpinnings of cancer cell chemoresponsiveness. NCI-H1155, a human non-small-cell lung cancer line, was employed in a paclitaxel-dependent synthetic lethal screen designed to identify gene targets that specifically reduce cell viability in the presence of otherwise sublethal concentrations of paclitaxel. Using a stringent objective statistical algorithm to reduce false discovery rates below 5%, we isolated a panel of 87 genes that represent major focal points of the autonomous response of cancer cells to the abrogation of microtubule dynamics. Here we show that several of these targets sensitize lung cancer cells to paclitaxel concentrations 1,000-fold lower than otherwise required for a significant response, and we identify mechanistic relationships between cancer-associated aberrant gene expression programmes and the basic cellular machinery required for robust mitotic progression.

Carcinoma, Non-Small-Cell Lung - pathology

Lung Neoplasms - genetics

Cell Survival - drug effects

Lung Neoplasms - drug therapy

RNA, Small Interfering - genetics

Lung - pathology

Paclitaxel - pharmacology

Carcinoma, Non-Small-Cell Lung - genetics

Humans

Spindle Apparatus - pathology

Lung Neoplasms - pathology

Dose-Response Relationship, Drug

Microtubules - metabolism

Mitosis - drug effects

Spindle Apparatus - metabolism

DNA Mutational Analysis

Microtubules - drug effects

Genes, Lethal - genetics

Lung - drug effects

Cell Line, Tumor

Lung - metabolism

Spindle Apparatus - drug effects

Carcinoma, Non-Small-Cell Lung - drug therapy

RNA, Small Interfering - metabolism

Details

Title: Subtitle: Synthetic lethal screen identification of chemosensitizer loci in cancer cells
Creators: Angelique W Whitehurst - Department of Cell Biology, University of Texas Southwestern Medical Center, Dallas, Texas 75390, USA
Brian O Bodemann
Jessica Cardenas
Deborah Ferguson
Luc Girard
Michael Peyton
John D Minna
Carolyn Michnoff
Weihua Hao
Michael G Roth
Xian-Jin Xie
Michael A White
Resource Type: Journal article
Publication Details: Nature (London), Vol.446(7137), pp.815-819
Publisher: England
DOI: 10.1038/nature05697
PMID: 17429401
ISSN: 1476-4687
eISSN: 1476-4687
Grant note: P50 CA070907 / NCI NIH HHS
Language: English
Date published: 04/12/2007
Academic Unit: Preventive and Community Dentistry; Biostatistics; Dental Research
Record Identifier: 9983917664502771

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