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Z-DNA is remodelled by ZBTB43 in prospermatogonia to safeguard the germline genome and epigenome

Authors :
Yingying Meng
Guliang Wang
Hongjuan He
Kin H. Lau
Allison Hurt
Brianna J. Bixler
Andrea Parham
Seung-Gi Jin
Xingzhi Xu
Karen M. Vasquez
Gerd P. Pfeifer
Piroska E. Szabó
Source :
Nature Cell Biology. 24:1141-1153
Publication Year :
2022
Publisher :
Springer Science and Business Media LLC, 2022.

Abstract

Mutagenic purine–pyrimidine repeats can adopt the left-handed Z-DNA conformation. DNA breaks at potential Z-DNA sites can lead to somatic mutations in cancer or to germline mutations that are transmitted to the next generation. It is not known whether any mechanism exists in the germ line to control Z-DNA structure and DNA breaks at purine–pyrimidine repeats. Here we provide genetic, epigenomic and biochemical evidence for the existence of a biological process that erases Z-DNA specifically in germ cells of the mouse male foetus. We show that a previously uncharacterized zinc finger protein, ZBTB43, binds to and removes Z-DNA, preventing the formation of DNA double-strand breaks. By removing Z-DNA, ZBTB43 also promotes de novo DNA methylation at CG-containing purine–pyrimidine repeats in prospermatogonia. Therefore, the genomic and epigenomic integrity of the species is safeguarded by remodelling DNA structure in the mammalian germ line during a critical window of germline epigenome reprogramming.

Subjects

Subjects :
Cell Biology

Details

ISSN :
14764679 and 14657392
Volume :
24
Database :
OpenAIRE
Journal :
Nature Cell Biology
Accession number :
edsair.doi...........d1996cc3ada790559e464820ae0a144f
Full Text :
https://doi.org/10.1038/s41556-022-00941-9