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Oncotarget

Epigenetically Guided Cancer Therapy: Targeting H3K27me3 Loss in Pediatric Brain Tumors

Aug 2, 2023
Dr. Michael Goldstein discusses targeting H3K27me3 loss in pediatric brain tumors, particularly DMG, ependymoma, and medulloblastoma. High relapse rates in pediatric cancer challenge current treatments, with radiotherapy as a primary modality. H3K27 tri-methylation is a key epigenetic trait in these brain tumors. Exploring the role of H3K27-Me3 in treatment response and survival rates.
03:40

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Quick takeaways

  • Global loss of H3K27 trimethylation in DMG is a hallmark, while aggressive PFA ependymoma subgroup lacks H3K27-Me3.
  • Deficiency in H3K27-Me3 in medulloblastoma correlates with high relapse rates and poor survival outcomes.

Deep dives

Distinct Epigenetic Traits of Pediatric Brain Tumors

High-grade tumors of the central nervous system in pediatric oncology, such as medulla blastoma, appendymoma, and DMG, pose significant challenges due to aggressive growth and high relapse rates. Dr. Michael Goldstein's editorial highlights distinct epigenetic traits of these tumors, emphasizing the global loss of H3K27 trimethylation (H3K27-Me3) in DMG and the lack of H3K27-Me3 in aggressive PFA appendymoma subgroup. While radiation is the primary treatment for DMG, tumors deficient in H3K27-Me3 are associated with high relapse rates and poor survival.

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