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

Publiceringsår

2005

Upphovspersoner

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

Abstrakt

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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Organisationer och upphovspersoner

Teknologiska forskningscentralen VTT Ab

Edgren Henrik

Wolf Maija

Kallioniemi Olli

Kilpinen Sami

Publikationstyp

Publikationsform

Artikel

Moderpublikationens typ

Tidning

Artikelstyp

En originalartikel

Målgrupp

Vetenskaplig

Kollegialt utvärderad

Kollegialt utvärderad

UKM:s publikationstyp

A1 Originalartikel i en vetenskaplig tidskrift

Publikationskanalens uppgifter

Journal/Serie

Cellular Oncology

Volym

27

Nummer

3

Sidor

169-173

Publikationsforum

53217

Publikationsforumsnivå

1

Öppen tillgång

Öppen tillgänglighet i förläggarens tjänst

Ja

Öppen tillgång till publikationskanalen

Helt öppen publikationskanal

Licens för förläggarens version

CC BY

Parallellsparad

Nej

Övriga uppgifter

Nyckelord

[object Object],[object Object],[object Object],[object Object],[object Object]

Språk

engelska

Internationell sampublikation

Ja

Sampublikation med ett företag

Nej

DOI

10.1155/2005/478316

Publikationen ingår i undervisnings- och kulturministeriets datainsamling

Nej