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Dissecting the precise role of H3K9 methylation in crosstalk with DNA maintenance methylation in mammals.


ABSTRACT: In mammals it is unclear if UHRF1-mediated DNA maintenance methylation by DNMT1 is strictly dependent on histone H3K9 methylation. Here we have generated an Uhrf1 knockin (KI) mouse model that specifically abolishes the H3K9me2/3-binding activity of Uhrf1. The homozygous Uhrf1 KI mice are viable and fertile, and exhibit ?10% reduction of DNA methylation in various tissues. The reduced DNA methylation occurs globally in the genome and does not restrict only to the H3K9me2/3 enriched repetitive sequences. In vitro UHRF1 binds with higher affinity to reconstituted nucleosome with hemi-methylated CpGs than that with H3K9me2/3, although it binds cooperatively to nucleosome with both modifications. We also show that the nucleosome positioning affects the binding of methylated DNA by UHRF1. Thus, while our study supports a role for H3K9 methylation in promoting DNA methylation, it demonstrates for the first time that DNA maintenance methylation in mammals is largely independent of H3K9 methylation.

SUBMITTER: Zhao Q 

PROVIDER: S-EPMC5426519 | biostudies-literature | 2016 Aug

REPOSITORIES: biostudies-literature

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Dissecting the precise role of H3K9 methylation in crosstalk with DNA maintenance methylation in mammals.

Zhao Qian Q   Zhang Jiqin J   Chen Ruoyu R   Wang Lina L   Li Bo B   Cheng Hao H   Duan Xiaoya X   Zhu Haijun H   Wei Wei W   Li Jiwen J   Wu Qihan Q   Han Jing-Dong J JD   Yu Wenqiang W   Gao Shaorong S   Li Guohong G   Wong Jiemin J  

Nature communications 20160824


In mammals it is unclear if UHRF1-mediated DNA maintenance methylation by DNMT1 is strictly dependent on histone H3K9 methylation. Here we have generated an Uhrf1 knockin (KI) mouse model that specifically abolishes the H3K9me2/3-binding activity of Uhrf1. The homozygous Uhrf1 KI mice are viable and fertile, and exhibit ∼10% reduction of DNA methylation in various tissues. The reduced DNA methylation occurs globally in the genome and does not restrict only to the H3K9me2/3 enriched repetitive se  ...[more]

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