Author:
Takahashi Nozomi,Coluccio Andrea,Thorball Christian W.,Planet Evarist,Shi Hui,Offner Sandra,Turelli Priscilla,Imbeault Michael,Ferguson-Smith Anne C.,Trono Didier
Abstract
Genomic imprinting is an epigenetic process regulated by germline-derived DNA methylation, causing parental origin-specific monoallelic gene expression. Zinc finger protein 57 (ZFP57) is critical for maintenance of this epigenetic memory during post-fertilization reprogramming, yet incomplete penetrance of ZFP57 mutations in humans and mice suggests additional effectors. We reveal that ZNF445/ZFP445, which we trace to the origins of imprinting, binds imprinting control regions (ICRs) in mice and humans. In mice, ZFP445 and ZFP57 act together, maintaining all but one ICR in vivo, whereas earlier embryonic expression of ZNF445 and its intolerance to loss-of-function mutations indicate greater importance in the maintenance of human imprints.
Funder
Herchel Smith Fellowship
Medical Research Council
Wellcome Trust
People Programme
Marie Curie Actions
European Union's Seventh Framework Programme
FP7 MC-ITN INGENIUM
Swiss National Science Foundation
European Research Council
Gebert-Rüf Foundation
Publisher
Cold Spring Harbor Laboratory
Subject
Developmental Biology,Genetics
Cited by
152 articles.
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