Cellular Oncology (Jan 2005)

NMD Microarray Analysis for Rapid Genome-Wide Screen of Mutated Genes in Cancer

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

DOI
https://doi.org/10.1155/2005/478316
Journal volume & issue
Vol. 27, no. 3
pp. 169 – 173

Abstract

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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 EPHB2 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.