Login / Signup

Pramel15 facilitates zygotic nuclear DNMT1 degradation and DNA demethylation.

Jiajun TanYingfeng LiXiang LiXiaoxiao ZhuLiping LiuHua HuangJiahua WeiHai-Lin WangYong TianZhigao WangZhuqiang ZhangBing Zhu
Published in: Nature communications (2024)
In mammals, global passive demethylation contributes to epigenetic reprogramming during early embryonic development. At this stage, the majority of DNA-methyltransferase 1 (DNMT1) protein is excluded from nucleus, which is considered the primary cause. However, whether the remaining nuclear activity of DNMT1 is regulated by additional mechanisms is unclear. Here, we report that nuclear DNMT1 abundance is finetuned through proteasomal degradation in mouse zygotes. We identify a maternal factor, Pramel15, which targets DNMT1 for degradation via Cullin-RING E3 ligases. Loss of Pramel15 elevates DNMT1 levels in the zygote pronuclei, impairs zygotic DNA demethylation, and causes a stochastic gain of DNA methylation in early embryos. Thus, Pramel15 can modulate the residual level of DNMT1 in the nucleus during zygotic DNA replication, thereby ensuring efficient DNA methylation reprogramming in early embryos.
Keyphrases
  • dna methylation
  • genome wide
  • gene expression
  • circulating tumor
  • cell free
  • single molecule
  • copy number
  • pregnant women
  • body mass index
  • weight loss
  • binding protein
  • amino acid
  • preterm birth
  • wastewater treatment