Haiyun Gan scite author profile

Recent studies have identified a Lys 27-to-methionine (K27M) mutation at one allele of H3F3A, one of the two genes encoding histone H3 variant H3.3, in 60% of high-grade pediatric glioma cases. The median survival of this group of patients after diagnosis is ~1 yr. Here we show that the levels of H3K27 di-and trimethylation (H3K27me2 and H3K27me3) are reduced globally in H3.3K27M patient samples due to the expression of the H3.3K27M mutant allele. Remarkably, we also observed that H3K27me3 and Ezh2 (the catalytic subunit of H3K27 methyltransfer-ase) at chromatin are dramatically increased locally at hundreds of gene loci in H3.3K27M patient cells. Moreover , the gain of H3K27me3 and Ezh2 at gene promoters alters the expression of genes that are associated with various cancer pathways. These results indicate that H3.3K27M mutation reprograms epigenetic landscape and gene expression, which may drive tumorigenesis.

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Pharmacologic inhibition of histone demethylation as a therapy for pediatric brainstem glioma

Hashizume

Andor

Ihara

et al. 2014

Nat Med

423

344

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A mechanism for preventing asymmetric histone segregation onto replicating DNA strands

Gan

Serra-Cardona

et al. 2018

Science

214

274

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How parental histone (H3-H4) tetramers, the primary carriers of epigenetic modifications, are transferred onto leading and lagging strands of DNA replication forks for epigenetic inheritance remains elusive. Here we show that parental (H3-H4) tetramers are assembled into nucleosomes onto both leading and lagging strands, with a slight preference for lagging strands. The lagging-strand preference increases markedly in budding yeast cells lacking Dpb3 and Dpb4, two subunits of the leading strand DNA polymerase, Pol ε, owing to the impairment of parental (H3-H4) transfer to leading strands. Dpb3-Dpb4 binds H3-H4 in vitro and participates in the inheritance of heterochromatin. These results indicate that different proteins facilitate the transfer of parental (H3-H4) onto leading versus lagging strands and that Dbp3-Dpb4 plays an important role in this poorly understood process.

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Haiyun Gan

The histone H3.3K27M mutation in pediatric glioma reprograms H3K27 methylation and gene expression

Pharmacologic inhibition of histone demethylation as a therapy for pediatric brainstem glioma

A mechanism for preventing asymmetric histone segregation onto replicating DNA strands

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