m6A facilitates hippocampus-dependent learning and memory through YTHDF1

被引:0
|
作者
Hailing Shi
Xuliang Zhang
Yi-Lan Weng
Zongyang Lu
Yajing Liu
Zhike Lu
Jianan Li
Piliang Hao
Yu Zhang
Feng Zhang
You Wu
Jary Y. Delgado
Yijing Su
Meera J. Patel
Xiaohua Cao
Bin Shen
Xingxu Huang
Guo-li Ming
Xiaoxi Zhuang
Hongjun Song
Chuan He
Tao Zhou
机构
[1] The University of Chicago,Department of Chemistry
[2] The University of Chicago,Department of Biochemistry and Molecular Biology
[3] The University of Chicago,Institute for Biophysical Dynamics
[4] The University of Chicago,Howard Hughes Medical Institute
[5] ShanghaiTech University,School of Life Science and Technology
[6] Zhejiang University,Laboratory Animal Center
[7] University of Pennsylvania,Department of Neuroscience Perelman School of Medicine
[8] Perelman School of Medicine,Mahoney Institute for Neurosciences
[9] University of Pennsylvania,School of Life Sciences and Technology
[10] Tongji University,Department of Neurobiology
[11] The University of Chicago,Key Laboratory of Brain Functional Genomics
[12] Ministry of Education,State Key Laboratory of Reproductive Medicine, Department of Histology and Embryology
[13] Shanghai Key Laboratory of Brain Functional Genomics,Department of Psychiatry, Perelman School of Medicine
[14] School of Life Sciences,Department of Cell and Developmental Biology
[15] East China Normal University,Institute for Regenerative Medicine
[16] Nanjing Medical University,The Epigenetics Institute, Perelman School of Medicine
[17] University of Pennsylvania,undefined
[18] Perelman School of Medicine,undefined
[19] University of Pennsylvania,undefined
[20] Perelman School of Medicine,undefined
[21] University of Pennsylvania,undefined
[22] University of Pennsylvania,undefined
来源
Nature | 2018年 / 563卷
关键词
Adult Mouse Hippocampus; Contextual Fear Memory; mM Methyl Methanethiosulfonate (MMTS); PBS With 0.1% Tween-20 (PBST); Protein Synthesis Assay;
D O I
暂无
中图分类号
学科分类号
摘要
N6-methyladenosine (m6A), the most prevalent internal RNA modification on mammalian messenger RNAs, regulates the fates and functions of modified transcripts through m6A-specific binding proteins1–5. In the nervous system, m6A is abundant and modulates various neural functions6–11. Whereas m6A marks groups of mRNAs for coordinated degradation in various physiological processes12–15, the relevance of m6A for mRNA translation in vivo remains largely unknown. Here we show that, through its binding protein YTHDF1, m6A promotes protein translation of target transcripts in response to neuronal stimuli in the adult mouse hippocampus, thereby facilitating learning and memory. Mice with genetic deletion of Ythdf1 show learning and memory defects as well as impaired hippocampal synaptic transmission and long-term potentiation. Re-expression of YTHDF1 in the hippocampus of adult Ythdf1-knockout mice rescues the behavioural and synaptic defects, whereas hippocampus-specific acute knockdown of Ythdf1 or Mettl3, which encodes the catalytic component of the m6A methyltransferase complex, recapitulates the hippocampal deficiency. Transcriptome-wide mapping of YTHDF1-binding sites and m6A sites on hippocampal mRNAs identified key neuronal genes. Nascent protein labelling and tether reporter assays in hippocampal neurons showed that YTHDF1 enhances protein synthesis in a neuronal-stimulus-dependent manner. In summary, YTHDF1 facilitates translation of m6A-methylated neuronal mRNAs in response to neuronal stimulation, and this process contributes to learning and memory.
引用
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页码:249 / 253
页数:4
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