Genetic variation at the 8q24.21 renal cancer susceptibility locus affects HIF binding to a MYC enhancer.
Steffen GramppJames L PlattVictoria LauerRafik SalamaFranziska KranzViviana K NeumannSven WachChristine StöhrArndt HartmannKai-Uwe EckardtPeter J RatcliffeDavid R MoleJohannes SchödelPublished in: Nature communications (2016)
Clear cell renal cell carcinoma (ccRCC) is characterized by loss of function of the von Hippel-Lindau tumour suppressor (VHL) and unrestrained activation of hypoxia-inducible transcription factors (HIFs). Genetic and epigenetic determinants have an impact on HIF pathways. A recent genome-wide association study on renal cancer susceptibility identified single-nucleotide polymorphisms (SNPs) in an intergenic region located between the oncogenes MYC and PVT1. Here using assays of chromatin conformation, allele-specific chromatin immunoprecipitation and genome editing, we show that HIF binding to this regulatory element is necessary to trans-activate MYC and PVT1 expression specifically in cells of renal tubular origins. Moreover, we demonstrate that the risk-associated polymorphisms increase chromatin accessibility and activity as well as HIF binding to the enhancer. These findings provide further evidence that genetic variation at HIF-binding sites modulates the oncogenic transcriptional output of the VHL-HIF axis and provide a functional explanation for the disease-associated effects of SNPs in ccRCC.
Keyphrases
- transcription factor
- endothelial cells
- genome wide
- genome editing
- crispr cas
- gene expression
- dna binding
- genome wide association study
- papillary thyroid
- dna methylation
- genome wide identification
- induced apoptosis
- poor prognosis
- binding protein
- squamous cell carcinoma
- young adults
- endoplasmic reticulum stress
- copy number
- cell death
- signaling pathway
- heat shock protein