Cancer Cell International (Sep 2007)

Modulation by decitabine of gene expression and growth of osteosarcoma U2OS cells <it>in vitro </it>and in xenografts: Identification of apoptotic genes as targets for demethylation

  • Xue Hui,
  • Cutz Jean-Claude,
  • Prasad Mona,
  • Bayani Jane,
  • Hughes Simon,
  • Somers Gino R,
  • Al-Romaih Khaldoun,
  • Zielenska Maria,
  • Wang Yuzhuo,
  • Squire Jeremy A

DOI
https://doi.org/10.1186/1475-2867-7-14
Journal volume & issue
Vol. 7, no. 1
p. 14

Abstract

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Abstract Background Methylation-mediated silencing of genes is one epigenetic mechanism implicated in cancer. Studies regarding the role of modulation of gene expression utilizing inhibitors of DNA methylation, such as decitabine, in osteosarcoma (OS) have been limited. A biological understanding of the overall effects of decitabine in OS is important because this particular agent is currently undergoing clinical trials. The objective of this study was to measure the response of the OS cell line, U2OS, to decitabine treatment both in vitro and in vivo. Results Microarray expression profiling was used to distinguish decitabine-dependent changes in gene expression in U2OS cells, and to identify responsive loci with demethylated CpG promoter regions. U2OS xenografts were established under the sub-renal capsule of immune-deficient mice to study the effect of decitabine in vivo on tumor growth and differentiation. Reduced nuclear methylation levels could be detected in xenografts derived from treated mice by immunohistochemistry utilizing a 5-methylcytidine antibody. Decitabine treatment reduced tumor xenograft size significantly (p in vitro (p GADD45A, HSPA9B, PAWR, PDCD5, NFKBIA, and TNFAIP3) were also induced to ≥2-fold in vivo. Quantitative methylation pyrosequencing confirmed that the tested pro-apoptotic genes had CpG-island DNA demethylationas a result of U2OS decitabine treatment both in vitro and in xenografts Conclusion These data provide new insights regarding the use of epigenetic modifiers in OS, and have important implications for therapeutic trials involving demethylation drugs. Collectively, these data have provided biological evidence that one mode of action of decitabine may be the induction of apoptosis utilizing promoter-CpG demethylation of specific effectors in cell death pathways in OS.