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NMD microarray analysis for rapid genome-wide screen of mutated genes in cancer

Year of publication

2005

Authors

Wolf, Maija; Edgren, Henrik; Muggerud, Aslaug; Kilpinen, Sami; Huusko, Pia; Sørlie, Therese; Mousses, Spyro; Kallioniemi, Olli

Abstract

Gene mutations play a critical role in cancer development and progression, and their identification offers possibilities for accurate diagnostics and therapeutic targeting. Finding genes undergoing mutations is challenging and slow, even in the post-genomic era. A new approach was recently developed by Noensie and Dietz to prioritize and focus the search, making use of nonsense-mediated mRNA decay (NMD) inhibition and microarray analysis (NMD microarrays) in the identification of transcripts containing nonsense mutations. We combined NMD microarrays with array-based CGH (comparative genomic hybridization) in order to identify inactivation of tumor suppressor genes in cancer. Such a “mutatomics” screening of prostate cancer cell lines led to the identification of inactivating mutations in the <em>EPHB2</em> gene. Up to 8% of metastatic uncultured prostate cancers also showed mutations of this gene whose loss of function may confer loss of tissue architecture. NMD microarray analysis could turn out to be a powerful research method to identify novel mutated genes in cancer cell lines, providing targets that could then be further investigated for their clinical relevance and therapeutic potential.
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Organizations and authors

VTT Technical Research Centre of Finland Ltd

Edgren Henrik

Wolf Maija

Kallioniemi Olli

Kilpinen Sami

Publication type

Publication format

Article

Parent publication type

Journal

Article type

Original article

Audience

Scientific

Peer-reviewed

Peer-Reviewed

MINEDU's publication type classification code

A1 Journal article (refereed), original research

Publication channel information

Journal/Series

Cellular Oncology

Volume

27

Issue

3

Pages

169-173

​Publication forum

53217

​Publication forum level

1

Open access

Open access in the publisher’s service

Yes

Open access of publication channel

Fully open publication channel

License of the publisher’s version

CC BY

Self-archived

No

Other information

Keywords

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Language

English

International co-publication

Yes

Co-publication with a company

No

DOI

10.1155/2005/478316

The publication is included in the Ministry of Education and Culture’s Publication data collection

No