Malignant rhabdoid tumours (MRT) are aggressive pediatric solid cancers driven by loss of SMARCB1. To study deregulated transcriptional and epigenetic regulatory networks in MRT, we perform integrative bioinformatics analyses of whole genome, transcriptome, miRNA, genome-wide DNA methylation and histone modifications in primary patient tissues and cell lines. Our analyses have revealed molecular heterogeneity in MRT, and shown evidence for deregulated pathways underpinning MRT pathology.

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