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CDCA7 is an evolutionarily conserved hemimethylated DNA sensor in eukaryotes

Isabel E. Wassing, Atsuya Nishiyama, Reia Shikimachi, Qingyuan Jia, Amika Kikuchi, Moeri Hiruta, Keita Sugimura, Xin Hong, Yoshie Chiba, Junhui Peng, Christopher Jenness, Makoto Nakanishi, Li Zhao, Kyohei Arita, Hironori Funabiki

2024Science Advances27 citationsDOIOpen Access PDF

Abstract

Mutations of the SNF2 family ATPase HELLS and its activator CDCA7 cause immunodeficiency, centromeric instability, and facial anomalies syndrome, characterized by DNA hypomethylation at heterochromatin. It remains unclear why CDCA7-HELLS is the sole nucleosome remodeling complex whose deficiency abrogates the maintenance of DNA methylation. We here identify the unique zinc-finger domain of CDCA7 as an evolutionarily conserved hemimethylation-sensing zinc finger (HMZF) domain. Cryo-electron microscopy structural analysis of the CDCA7-nucleosome complex reveals that the HMZF domain can recognize hemimethylated CpG in the outward-facing DNA major groove within the nucleosome core particle, whereas UHRF1, the critical activator of the maintenance methyltransferase DNMT1, cannot. CDCA7 recruits HELLS to hemimethylated chromatin and facilitates UHRF1-mediated H3 ubiquitylation associated with replication-uncoupled maintenance DNA methylation. We propose that the CDCA7-HELLS nucleosome remodeling complex assists the maintenance of DNA methylation on chromatin by sensing hemimethylated CpG that is otherwise inaccessible to UHRF1 and DNMT1.

Topics & Concepts

ChromatinNucleosomeDNA methylationBiologyHeterochromatinHistoneCell biologyDNAGeneticsChromatin remodelingDNA repairGeneGene expressionEpigenetics and DNA MethylationRNA modifications and cancerCancer-related gene regulation