Mettl14 is Required for Mouse Postimplantation Development by Facilitating Epiblast Maturation

Overview

Journal FASEB J

Specialties Biology
Physiology

Date 2018 Aug 16

PMID 30110177

Citations 46

Authors

Tie-Gang Meng

Xukun Lu

Lei Guo

Guan-Mei Hou

Xue-Shan Ma

Qian-Nan Li

Lin Huang

Li-Hua Fan

Zheng-Hui Zhao

Xiang-Hong Ou

Ying-Chun Ouyang

Heide Schatten

Lei Li

Zhen-Bo Wang

Qing-Yuan Sun

Affiliations

Soon will be listed here.

Abstract

N6-methyladenosine (mA) is the most prevalent and reversible internal modification of mammalian messenger and noncoding RNAs mediated by specific mA writer, reader, and eraser proteins. As an mA writer, the methyltransferase-like 3-methyltransferase-like 14 (METTL14)-Wilms tumor 1-associated protein complex dynamically regulates mA modification and plays important roles in diverse biologic processes. However, our knowledge about the complete functions of this RNA methyltransferase complex, the contributions of each component to the methylation, and their effects on different biologic pathways are still limited. By using both in vivo and in vitro models, we here report that METTL14 is indispensable for postimplantation embryonic development by facilitating the conversion from naive to primed state of the epiblast. Depletion of Mettl14 leads to conspicuous embryonic growth retardation from embryonic d 6.5, mainly as a result of resistance to differentiation, which further leads to embryonic lethality early in gestation. Our data highlight the critical function of METTL14 as an mA modification regulator in orchestrating early mouse embryogenesis.-Meng, T.-G., Lu, X., Guo, L., Hou, G.-M., Ma, X.-S., Li, Q.-N., Huang, L., Fan, L.-H., Zhao, Z.-H., Ou, X.-H., OuYang, Y.-C., Schatten, H., Li, L., Wang, Z.-B., Sun, Q.-Y. Mettl14 is required for mouse postimplantation development by facilitating epiblast maturation.

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