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Targeting epigenetic aberrations of sarcoma in CRISPR era.

Miwa TanakaTakuro Nakamura
Published in: Genes, chromosomes & cancer (2023)
Sarcomas are rare malignancies that exhibit diverse biological, genetic, morphological and clinical characteristics. Genetic alterations, such as gene fusions, mutations in transcriptional machinery components, histones, and DNA methylation regulatory molecules, play an essential role in sarcomagenesis. These mutations induce and/or cooperate with specific epigenetic aberrations required for the growth and maintenance of sarcomas. Appropriate mouse models have been developed to clarify the significance of genetic and epigenetic interactions in sarcomas. Studies using the mouse models for human sarcomas have demonstrated major advances in our understanding the developmental processes as well as tumor microenvironment of sarcomas. Recent technological progresses in epigenome editing will not only improve the studies using animal models but also provide a direct clue for epigenetic therapies. In this manuscript, we review important epigenetic aberrations in sarcomas and their representative mouse models, current methods of epigenetic editing using CRISPR/dCas9 systems, and potential applications in sarcoma studies and therapeutics.
Keyphrases
  • dna methylation
  • genome wide
  • copy number
  • gene expression
  • high grade
  • crispr cas
  • mouse model
  • genome editing
  • transcription factor
  • endothelial cells
  • climate change
  • oxidative stress
  • cancer therapy
  • human health