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JMJD3 acts in tandem with KLF4 to facilitate reprogramming to pluripotency.


ABSTRACT: The interplay between the Yamanaka factors (OCT4, SOX2, KLF4 and c-MYC) and transcriptional/epigenetic co-regulators in somatic cell reprogramming is incompletely understood. Here, we demonstrate that the histone H3 lysine 27 trimethylation (H3K27me3) demethylase JMJD3 plays conflicting roles in mouse reprogramming. On one side, JMJD3 induces the pro-senescence factor Ink4a and degrades the pluripotency regulator PHF20 in a reprogramming factor-independent manner. On the other side, JMJD3 is specifically recruited by KLF4 to reduce H3K27me3 at both enhancers and promoters of epithelial and pluripotency genes. JMJD3 also promotes enhancer-promoter looping through the cohesin loading factor NIPBL and ultimately transcriptional elongation. This competition of forces can be shifted towards improved reprogramming by using early passage fibroblasts or boosting JMJD3's catalytic activity with vitamin C. Our work, thus, establishes a multifaceted role for JMJD3, placing it as a key partner of KLF4 and a scaffold that assists chromatin interactions and activates gene transcription.

SUBMITTER: Huang Y 

PROVIDER: S-EPMC7545202 | biostudies-literature | 2020 Oct

REPOSITORIES: biostudies-literature

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JMJD3 acts in tandem with KLF4 to facilitate reprogramming to pluripotency.

Huang Yinghua Y   Zhang Hui H   Wang Lulu L   Tang Chuanqing C   Qin Xiaogan X   Wu Xinyu X   Pan Meifang M   Tang Yujia Y   Yang Zhongzhou Z   Babarinde Isaac A IA   Lin Runxia R   Ji Guanyu G   Lai Yiwei Y   Xu Xueting X   Su Jianbin J   Wen Xue X   Satoh Takashi T   Ahmed Tanveer T   Malik Vikas V   Ward Carl C   Volpe Giacomo G   Guo Lin L   Chen Jinlong J   Sun Li L   Li Yingying Y   Huang Xiaofen X   Bao Xichen X   Gao Fei F   Liu Baohua B   Zheng Hui H   Jauch Ralf R   Lai Liangxue L   Pan Guangjin G   Chen Jiekai J   Testa Giuseppe G   Akira Shizuo S   Hu Jifan J   Pei Duanqing D   Hutchins Andrew P AP   Esteban Miguel A MA   Qin Baoming B  

Nature communications 20201008 1


The interplay between the Yamanaka factors (OCT4, SOX2, KLF4 and c-MYC) and transcriptional/epigenetic co-regulators in somatic cell reprogramming is incompletely understood. Here, we demonstrate that the histone H3 lysine 27 trimethylation (H3K27me3) demethylase JMJD3 plays conflicting roles in mouse reprogramming. On one side, JMJD3 induces the pro-senescence factor Ink4a and degrades the pluripotency regulator PHF20 in a reprogramming factor-independent manner. On the other side, JMJD3 is spe  ...[more]

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