Integrated Functional, Gene Expression and Genomic Analysis for the Identification of Cancer Targets

Overview

Journal PLoS One

Specialties General Medicine
Science

Date 2009 Apr 10

PMID 19357772

Citations 65

Authors

Elizabeth Iorns

Christopher J Lord

Anita Grigoriadis

Sarah McDonald

Kerry Fenwick

Alan Mackay

Charles A Mein

Rachael Natrajan

Kay Savage

Narinder Tamber

Jorge S Reis-Filho

Nicholas C Turner

Alan Ashworth

Affiliations

Soon will be listed here.

Abstract

The majority of new drug approvals for cancer are based on existing therapeutic targets. One approach to the identification of novel targets is to perform high-throughput RNA interference (RNAi) cellular viability screens. We describe a novel approach combining RNAi screening in multiple cell lines with gene expression and genomic profiling to identify novel cancer targets. We performed parallel RNAi screens in multiple cancer cell lines to identify genes that are essential for viability in some cell lines but not others, suggesting that these genes constitute key drivers of cellular survival in specific cancer cells. This approach was verified by the identification of PIK3CA, silencing of which was selectively lethal to the MCF7 cell line, which harbours an activating oncogenic PIK3CA mutation. We combined our functional RNAi approach with gene expression and genomic analysis, allowing the identification of several novel kinases, including WEE1, that are essential for viability only in cell lines that have an elevated level of expression of this kinase. Furthermore, we identified a subset of breast tumours that highly express WEE1 suggesting that WEE1 could be a novel therapeutic target in breast cancer. In conclusion, this strategy represents a novel and effective strategy for the identification of functionally important therapeutic targets in cancer.

Citing Articles

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Pharmacoproteogenomic approach identifies on-target kinase inhibitors for cancer drug repositioning.

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High WEE1 expression is independently linked to poor survival in multiple myeloma.

Simhal A, Firestone R, Oh J, Avutu V, Norton L, Hultcrantz M bioRxiv. 2024; .

PMID: 39386721 PMC: 11463642. DOI: 10.1101/2024.09.20.613788.

Targeting WEE1 Kinase in Gynecological Malignancies.

Zhang W, Li Q, Yin R Drug Des Devel Ther. 2024; 18:2449-2460.

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METTL3 Promotes OSCC Progression by Down-Regulating WEE1 in a m6A-YTHDF2-Dependent Manner.

Su Y, Hu Y, Qu B, Lei R, Guo G Mol Biotechnol. 2024; .

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