Expression Profiling Combined with Epigenetic Scanning Microsatellite Instability Colon Carcinogenesis by Identification of Genes Uniquely Involved in Frequent

نویسندگان

  • Yuriko Mori
  • Jing Yin
  • Fumiaki Sato
  • Anca Sterian
  • Lisa A. Simms
  • Florin M. Selaru
  • Karsten Schulmann
  • Yan Xu
  • Andreea Olaru
  • Suna Wang
  • Elena Deacu
  • John M. Abraham
  • Joanne Young
  • Barbara A. Leggett
  • Stephen J. Meltzer
چکیده

Gene silencing through CpG island hypermethylation has been associated with genesis or progression of frequent microsatellite instability (MSI-H) cancers. To identify novel methylation sites unique to MSI-H colon cancers in an unbiased fashion, we conducted a global expression profiling-based methylation target search. We identified 81 genes selectively down-regulated in MSI-H cancers using cDNA microarray analysis of 41 primary colon cancers. Forty six of these 81 genes contained CpG islands overlapping their 5 untranslated regions. Initial screening of six genes in 57 primary colon cancers detected the following gene with MSI-H cancer-specific hypermethylation: RAB32, a ras family member and A-kinase-anchoring protein, was methylated in 14 of 25 (56%) MSI-H cancers but in none of 32 non-MSI-H cancers or 23 normal colonic specimens. RAB32 hypermethylation correlated with RAB32 mRNA down-regulation and with hMLH1 hypermethylation. In addition, the protein-tyrosine phosphatase receptor type O gene, PTPRO, was frequently methylated in rightsided tumors. This methylation screening strategy should identify additional genes inactivated by epigenetic silencing in colorectal and other cancers.

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تاریخ انتشار 2004