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Diverse Functions of KDM5 in Cancer: Transcriptional Repressor or Activator?

Yasuyo Ohguchi, Hiroto Ohguchi

2022Cancers33 citationsDOIOpen Access PDF

Abstract

Epigenetic modifications are crucial for chromatin remodeling and transcriptional regulation. Post-translational modifications of histones are epigenetic processes that are fine-tuned by writer and eraser enzymes, and the disorganization of these enzymes alters the cellular state, resulting in human diseases. The KDM5 family is an enzymatic family that removes di- and tri-methyl groups (me2 and me3) from lysine 4 of histone H3 (H3K4), and its dysregulation has been implicated in cancer. Although H3K4me3 is an active chromatin marker, KDM5 proteins serve as not only transcriptional repressors but also transcriptional activators in a demethylase-dependent or -independent manner in different contexts. Notably, KDM5 proteins regulate the H3K4 methylation cycle required for active transcription. Here, we review the recent findings regarding the mechanisms of transcriptional regulation mediated by KDM5 in various contexts, with a focus on cancer, and further shed light on the potential of targeting KDM5 for cancer therapy.

Topics & Concepts

DemethylaseEpigeneticsH3K4me3ChromatinHistoneTranscriptional regulationBiologyRepressorCell biologyHistone methylationTranscription factorGeneticsDNA methylationPromoterGene expressionGeneEpigenetics and DNA MethylationGenomics and Chromatin DynamicsChromatin Remodeling and Cancer
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