Molecular Cancer (Jun 2009)

CpG methylation profiling in <it>VHL </it>related and <it>VHL </it>unrelated renal cell carcinoma

  • Clarke Noel W,
  • Ragoussis Jiannis,
  • Baban Dilair,
  • Winchester Laura,
  • Gentle Dean,
  • Morris Mark R,
  • McRonald Fiona E,
  • Brown Michael D,
  • Kishida Takeshi,
  • Yao Masahiro,
  • Latif Farida,
  • Maher Eamonn R

DOI
https://doi.org/10.1186/1476-4598-8-31
Journal volume & issue
Vol. 8, no. 1
p. 31

Abstract

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Abstract Background Renal cell carcinoma (RCC) is histopathologically heterogeneous with clear cell and papillary the most common subtypes. The most frequent molecular abnormality in clear cell RCC is VHL inactivation but promoter methylation of tumour suppressor genes is common in both subtypes of RCC. To investigate whether RCC CpG methylation status was influenced by histopathology and VHL status we performed high-throughput epigenetic profiling using the Illumina Goldengate Methylation Array in 62 RCC (29 RCC from von Hippel-Lindau (VHL) disease patients, 20 sporadic clear cell RCC with wild type VHL and 13 sporadic papillary RCC). Results 43 genes were methylated in >20% of primary RCC (range 20–45%) and most (37/43) of these had not been reported previously to be methylated in RCC. The distribution of the number of methylated CpGs in individual tumours differed from the expected Poisson distribution (p Conclusion These findings demonstrate differing patterns of tumour-specific CpG methylation in VHL and non VHL clear cell RCC and papillary RCC, and identify multiple novel potential CpG methylation biomarkers for RCC.