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Epigenome Programming by H3.3K27M Mutation Creates a Dependence of Pediatric Glioma on SMARCA4.

Yan MoShou-Fu DuanXu ZhangXu HuaHui ZhouHong-Jian WeiJun WatanabeNicholas McQuillanZhenyi SuWei GuCheng-Chia WuChristopher R VakocRintaro HashizumeKenneth ChangZhiguo Zhang
Published in: Cancer discovery (2022)
DMG is a deadly pediatric glioma currently without effective treatments. We discovered that the chromatin remodeler SMARCA4 is essential for the proliferation of DMG with H3K27M mutation in vitro and in vivo, identifying a potentially novel therapeutic approach to this disease. See related commentary by Beytagh and Weiss, p. 2730. See related article by Panditharatna et al., p. 2880. This article is highlighted in the In This Issue feature, p. 2711.
Keyphrases
  • dna methylation
  • signaling pathway
  • machine learning
  • dna damage
  • genome wide
  • transcription factor