Integrative analysis reveals relationships of genetic and epigenetic alterations in osteosarcoma

Stine H Kresse; Halfdan Rydbeck; Magne Skårn; Heidi M Namløs; Ana H Barragan-Polania; Anne-Marie Cleton-Jansen; Massimo Serra; Knut Liestøl; Pancras C W Hogendoorn; Eivind Hovig; Ola Myklebost; Leonardo A Meza-Zepeda

doi:10.1371/journal.pone.0048262

Integrative analysis reveals relationships of genetic and epigenetic alterations in osteosarcoma

PLoS One. 2012;7(11):e48262. doi: 10.1371/journal.pone.0048262. Epub 2012 Nov 7.

Authors

Stine H Kresse¹, Halfdan Rydbeck, Magne Skårn, Heidi M Namløs, Ana H Barragan-Polania, Anne-Marie Cleton-Jansen, Massimo Serra, Knut Liestøl, Pancras C W Hogendoorn, Eivind Hovig, Ola Myklebost, Leonardo A Meza-Zepeda

Affiliation

¹ Department of Tumour Biology, The Norwegian Radium Hospital, Oslo University Hospital, Oslo, Norway.

Abstract

Background: Osteosarcomas are the most common non-haematological primary malignant tumours of bone, and all conventional osteosarcomas are high-grade tumours showing complex genomic aberrations. We have integrated genome-wide genetic and epigenetic profiles from the EuroBoNeT panel of 19 human osteosarcoma cell lines based on microarray technologies.

Principal findings: The cell lines showed complex patterns of DNA copy number changes, where genomic copy number gains were significantly associated with gene-rich regions and losses with gene-poor regions. By integrating the datasets, 350 genes were identified as having two types of aberrations (gain/over-expression, hypo-methylation/over-expression, loss/under-expression or hyper-methylation/under-expression) using a recurrence threshold of 6/19 (>30%) cell lines. The genes showed in general alterations in either DNA copy number or DNA methylation, both within individual samples and across the sample panel. These 350 genes are involved in embryonic skeletal system development and morphogenesis, as well as remodelling of extracellular matrix. The aberrations of three selected genes, CXCL5, DLX5 and RUNX2, were validated in five cell lines and five tumour samples using PCR techniques. Several genes were hyper-methylated and under-expressed compared to normal osteoblasts, and expression could be reactivated by demethylation using 5-Aza-2'-deoxycytidine treatment for four genes tested; AKAP12, CXCL5, EFEMP1 and IL11RA. Globally, there was as expected a significant positive association between gain and over-expression, loss and under-expression as well as hyper-methylation and under-expression, but gain was also associated with hyper-methylation and under-expression, suggesting that hyper-methylation may oppose the effects of increased copy number for detrimental genes.

Conclusions: Integrative analysis of genome-wide genetic and epigenetic alterations identified dependencies and relationships between DNA copy number, DNA methylation and mRNA expression in osteosarcomas, contributing to better understanding of osteosarcoma biology.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Bone Neoplasms / genetics*
Cell Line, Tumor
Cluster Analysis
DNA Copy Number Variations
DNA Methylation
Epigenesis, Genetic*
Gene Dosage
Gene Expression Regulation, Neoplastic*
Genes, Neoplasm
Genome-Wide Association Study
Humans
Oligonucleotide Array Sequence Analysis
Osteosarcoma / genetics*
Polymorphism, Single Nucleotide
RNA, Messenger / genetics
RNA, Messenger / metabolism

Substances

RNA, Messenger

Grants and funding

This work was supported by the European Network to Promote Research into Uncommon Cancers in Adults and Children: Pathology, Biology and Genetics of Bone Tumours (EuroBoNeT), the Norwegian Cancer Society (Ragnvarda F. Sørvik and Håkon Starheim’s legacy) and the Norwegian Research Council. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.