iScience (Aug 2024)

Reorganization of H3K9me heterochromatin leads to neuronal impairment via the cascading destruction of the KDM3B-centered epigenomic network

  • Mi-Jin An,
  • Ji-Young Kim,
  • Jinho Kim,
  • Dae-Hyun Kim,
  • Geun-Seup Shin,
  • Hyun-Min Lee,
  • Ah-Ra Jo,
  • Yuna Park,
  • Yujeong Hwangbo,
  • Chul-Hong Kim,
  • Mi Jin Kim,
  • Youn-Sang Jung,
  • Jeongkyu Kim,
  • Sangmyung Rhee,
  • Sang-Beom Seo,
  • Jung-Woong Kim

Journal volume & issue
Vol. 27, no. 8
p. 110380

Abstract

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Summary: Histone H3K9 methylated heterochromatin silences repetitive non-coding sequences and lineage-specific genes during development, but how tissue-specific genes escape from heterochromatin in differentiated cells is unclear. Here, we examine age-dependent transcriptomic profiling of terminally differentiated mouse retina to identify epigenetic regulators involved in heterochromatin reorganization. The single-cell RNA sequencing analysis reveals a gradual downregulation of Kdm3b in cone photoreceptors during aging. Disruption of Kdm3b (Kdm3b+/−) of 12-month-old mouse retina leads to the decreasing number of cones via apoptosis, and it changes the morphology of cone ribbon synapses. Integration of the transcriptome with epigenomic analysis in Kdm3b+/− retinas demonstrates gains of heterochromatin features in synapse assembly and vesicle transport genes that are downregulated via the accumulation of H3K9me1/2. Contrarily, losses of heterochromatin in apoptotic genes exacerbated retinal neurodegeneration. We propose that the KDM3B-centered epigenomic network is crucial for balancing of cone photoreceptor homeostasis via the modulation of gene set-specific heterochromatin features during aging.

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