Publication | Open Access
Integrative analysis of HIF binding and transactivation reveals its role in maintaining histone methylation homeostasis
403
Citations
33
References
2009
Year
Histone ModificationsEpigenetic ChangeGeneticsDna MethylationMolecular BiologyIntegrative AnalysisRedox BiologyEpigeneticsTranscriptional RegulationRedox RegulatorHistone Methylation HomeostasisHypoxia (Medicine)Cellular HypoxiaHypoxia-inducible Factor 1Gene ExpressionEpigenetic RegulationCell BiologyHif BindingChromatinChromatin RemodelingNatural SciencesEpigenomicsMedicine
Adaptation to hypoxia is mediated through a coordinated transcriptional response driven largely by hypoxia-inducible factor 1 (HIF-1). We used ChIP-chip and gene expression profiling to identify direct targets of HIF-1 transactivation on a genome-wide scale. Several hundred direct HIF-1 targets were identified and, as expected, were highly enriched for proteins that facilitate metabolic adaptation to hypoxia. Surprisingly, there was also striking enrichment for the family of 2-oxoglutarate dioxygenases, including the jumonji-domain histone demethylases. We demonstrate that these histone demethylases are direct HIF targets, and their up-regulation helps maintain epigenetic homeostasis under hypoxic conditions. These results suggest that the coordinated increase in expression of several oxygen-dependent enzymes by HIF may help compensate for decreased levels of oxygen under conditions of cellular hypoxia.
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