Recent evolution of a TET-controlled and DPPA3/STELLA-driven pathway of passive DNA demethylation in mammals

Author:

Mulholland Christopher B.ORCID,Nishiyama AtsuyaORCID,Ryan JoelORCID,Nakamura Ryohei,Yiğit Merve,Glück Ivo M.,Trummer Carina,Qin Weihua,Bartoschek Michael D.ORCID,Traube Franziska R.ORCID,Parsa Edris,Ugur Enes,Modic Miha,Acharya AishwaryaORCID,Stolz PaulORCID,Ziegenhain Christoph,Wierer MichaelORCID,Enard Wolfgang,Carell ThomasORCID,Lamb Don C.ORCID,Takeda HiroyukiORCID,Nakanishi MakotoORCID,Bultmann SebastianORCID,Leonhardt HeinrichORCID

Abstract

AbstractGenome-wide DNA demethylation is a unique feature of mammalian development and naïve pluripotent stem cells. Here, we describe a recently evolved pathway in which global hypomethylation is achieved by the coupling of active and passive demethylation. TET activity is required, albeit indirectly, for global demethylation, which mostly occurs at sites devoid of TET binding. Instead, TET-mediated active demethylation is locus-specific and necessary for activating a subset of genes, including the naïve pluripotency and germline marker Dppa3 (Stella, Pgc7). DPPA3 in turn drives large-scale passive demethylation by directly binding and displacing UHRF1 from chromatin, thereby inhibiting maintenance DNA methylation. Although unique to mammals, we show that DPPA3 alone is capable of inducing global DNA demethylation in non-mammalian species (Xenopus and medaka) despite their evolutionary divergence from mammals more than 300 million years ago. Our findings suggest that the evolution of Dppa3 facilitated the emergence of global DNA demethylation in mammals.

Funder

Deutsche Forschungsgemeinschaft

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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