| Literature DB >> 33500348 |
Weijun Jiang1,2,3, Jiajia Shi1, Jingjie Zhao1, Qiu Wang2, Dan Cong1, Fenghua Chen1, Yu Zhang4, Yuhan Liu1, Junzheng Zhao1, Qian Chen1, Linhao Gu1, Wenjia Zhou1, Chenhang Wang1, Zhaoyuan Fang2, Shuhui Geng1, Wei Xie4, Luo-Nan Chen1,2, Yang Yang1, Yun Bai5, Haodong Lin6, Xiajun Li5.
Abstract
ZFP57 is a master regulator of genomic imprinting. It has both maternal and zygotic functions that are partially redundant in maintaining DNA methylation at some imprinting control regions (ICRs). In this study, we found that DNA methylation was lost at most known ICRs in Zfp57 mutant embryos. Furthermore, loss of ZFP57 caused loss of parent-of-origin-dependent monoallelic expression of the target imprinted genes. The allelic expression switch occurred in the ZFP57 target imprinted genes upon loss of differential DNA methylation at the ICRs in Zfp57 mutant embryos. Specifically, upon loss of ZFP57, the alleles of the imprinted genes located on the same chromosome with the originally methylated ICR switched their expression to mimic their counterparts on the other chromosome with unmethylated ICR. Consistent with our previous study, ZFP57 could regulate the NOTCH signaling pathway in mouse embryos by impacting allelic expression of a few regulators in the NOTCH pathway. In addition, the imprinted Dlk1 gene that has been implicated in the NOTCH pathway was significantly down-regulated in Zfp57 mutant embryos. Our allelic expression switch models apply to the examined target imprinted genes controlled by either maternally or paternally methylated ICRs. Our results support the view that ZFP57 controls imprinted expression of its target imprinted genes primarily through maintaining differential DNA methylation at the ICRs.Entities:
Keywords: COBRA; RNA-seq; allelic expression; bisulfite sequencing; genomic imprinting
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Year: 2021 PMID: 33500348 PMCID: PMC7865185 DOI: 10.1073/pnas.2005377118
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205