MiR-199a Links MeCP2 with mTOR Signaling and Its Dysregulation Leads to Rett Syndrome Phenotypes

Keita Tsujimura; Koichiro Irie; Hideyuki Nakashima; Yoshihiro Egashira; Yoichiro Fukao; Masayuki Fujiwara; Masayuki Itoh; Masahiro Uesaka; Takuya Imamura; Yasukazu Nakahata; Yui Yamashita; Takaya Abe; Shigeo Takamori; Kinichi Nakashima

doi:10.1016/j.celrep.2015.08.028

MiR-199a Links MeCP2 with mTOR Signaling and Its Dysregulation Leads to Rett Syndrome Phenotypes

Keita Tsujimura, Koichiro Irie, Hideyuki Nakashima, Yoshihiro Egashira, Yoichiro Fukao, Masayuki Fujiwara, Masayuki Itoh, Masahiro Uesaka, Takuya Imamura, Yasukazu Nakahata, Yui Yamashita, Takaya Abe, Shigeo Takamori, Kinichi Nakashima^*

^*この研究の対応する著者

研究成果: Article › 査読

74 被引用数 (Scopus)

抄録

Rett syndrome (RTT) is a neurodevelopmental disorder caused by MECP2 mutations. Although emerging evidence suggests that MeCP2 deficiency is associated with dysregulation of mechanistic target of rapamycin (mTOR), which functions as a hub for various signaling pathways, the mechanism underlying this association and the molecular pathophysiology of RTT remain elusive. We show here that MeCP2 promotes the posttranscriptional processing of particular microRNAs (miRNAs) as a component of the microprocessor Drosha complex. Among the MeCP2-regulated miRNAs, we found that miR-199a positively controls mTOR signaling by targeting inhibitors for mTOR signaling. miR-199a and its targets have opposite effects on mTOR activity, ameliorating and inducing RTT neuronal phenotypes, respectively. Furthermore, genetic deletion of miR-199a-2 led to a reduction of mTOR activity in the brain and recapitulated numerous RTT phenotypes in mice. Together, these findings establish miR-199a as a critical downstream target of MeCP2 in RTT pathogenesis by linking MeCP2 with mTOR signaling.

本文言語	English
ページ（範囲）	1887-1901
ページ数	15
ジャーナル	Cell Reports
巻	12
号	11
DOI	https://doi.org/10.1016/j.celrep.2015.08.028
出版ステータス	Published - 2015 9月 22
外部発表	はい

ASJC Scopus subject areas

生化学、遺伝学、分子生物学（全般）

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10.1016/j.celrep.2015.08.028

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@article{3af597713b2741b0bf54dded0e70f460,

title = "MiR-199a Links MeCP2 with mTOR Signaling and Its Dysregulation Leads to Rett Syndrome Phenotypes",

abstract = "Rett syndrome (RTT) is a neurodevelopmental disorder caused by MECP2 mutations. Although emerging evidence suggests that MeCP2 deficiency is associated with dysregulation of mechanistic target of rapamycin (mTOR), which functions as a hub for various signaling pathways, the mechanism underlying this association and the molecular pathophysiology of RTT remain elusive. We show here that MeCP2 promotes the posttranscriptional processing of particular microRNAs (miRNAs) as a component of the microprocessor Drosha complex. Among the MeCP2-regulated miRNAs, we found that miR-199a positively controls mTOR signaling by targeting inhibitors for mTOR signaling. miR-199a and its targets have opposite effects on mTOR activity, ameliorating and inducing RTT neuronal phenotypes, respectively. Furthermore, genetic deletion of miR-199a-2 led to a reduction of mTOR activity in the brain and recapitulated numerous RTT phenotypes in mice. Together, these findings establish miR-199a as a critical downstream target of MeCP2 in RTT pathogenesis by linking MeCP2 with mTOR signaling.",

author = "Keita Tsujimura and Koichiro Irie and Hideyuki Nakashima and Yoshihiro Egashira and Yoichiro Fukao and Masayuki Fujiwara and Masayuki Itoh and Masahiro Uesaka and Takuya Imamura and Yasukazu Nakahata and Yui Yamashita and Takaya Abe and Shigeo Takamori and Kinichi Nakashima",

note = "Funding Information: We thank H. Sasaki, H. Tou, H. Suzuki, K. Yanagitani, and K. Miyake for technical advice and reagents. We also thank K. Kohno, K. Miyazono, M.E. Greenberg, Z. Zhou, and T. Kubota for sharing reagents and cells, I. Smith for editing the manuscript, and all members of the Department of Stem Cell Biology and Medicine, Kyushu University, of the Laboratory of Molecular Neuroscience, of the Laboratory of Gene Regulation Research, Nara Institute of Science and Technology (NAIST), and of the Laboratory of Neural Membrane Biology, Doshisha University for assistance. We appreciate the technical assistance from The Research Support Center, Kyushu University. We are grateful to the Harvard Brain Tissue Resource Center for providing RTT samples. This work was supported in part by a Grant-in-Aid for Scientific Research (grant no. 24240051), a Grant-in-Aid for Scientific Research on Innovative Area: Foundation of Synapse and Neurocircuit Pathology, and the NAIST Global COE Program (Frontier biosciences: strategies for survival and adaptation in a changing global environment), all from the Ministry of Education, Culture, Sports, Science and Technology of Japan; and by an Intramural Research Grant (24-12) for Neurological and Psychiatric Disorders of NCNP. This work was partly performed in the Cooperative Research Project Program of the Medical Institute of Bioregulation, Kyushu University. Publisher Copyright: {\textcopyright} 2015 The Authors.",

year = "2015",

month = sep,

day = "22",

doi = "10.1016/j.celrep.2015.08.028",

language = "English",

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T1 - MiR-199a Links MeCP2 with mTOR Signaling and Its Dysregulation Leads to Rett Syndrome Phenotypes

AU - Tsujimura, Keita

AU - Irie, Koichiro

AU - Nakashima, Hideyuki

AU - Egashira, Yoshihiro

AU - Fukao, Yoichiro

AU - Fujiwara, Masayuki

AU - Itoh, Masayuki

AU - Uesaka, Masahiro

AU - Imamura, Takuya

AU - Nakahata, Yasukazu

AU - Yamashita, Yui

AU - Abe, Takaya

AU - Takamori, Shigeo

AU - Nakashima, Kinichi

N1 - Funding Information: We thank H. Sasaki, H. Tou, H. Suzuki, K. Yanagitani, and K. Miyake for technical advice and reagents. We also thank K. Kohno, K. Miyazono, M.E. Greenberg, Z. Zhou, and T. Kubota for sharing reagents and cells, I. Smith for editing the manuscript, and all members of the Department of Stem Cell Biology and Medicine, Kyushu University, of the Laboratory of Molecular Neuroscience, of the Laboratory of Gene Regulation Research, Nara Institute of Science and Technology (NAIST), and of the Laboratory of Neural Membrane Biology, Doshisha University for assistance. We appreciate the technical assistance from The Research Support Center, Kyushu University. We are grateful to the Harvard Brain Tissue Resource Center for providing RTT samples. This work was supported in part by a Grant-in-Aid for Scientific Research (grant no. 24240051), a Grant-in-Aid for Scientific Research on Innovative Area: Foundation of Synapse and Neurocircuit Pathology, and the NAIST Global COE Program (Frontier biosciences: strategies for survival and adaptation in a changing global environment), all from the Ministry of Education, Culture, Sports, Science and Technology of Japan; and by an Intramural Research Grant (24-12) for Neurological and Psychiatric Disorders of NCNP. This work was partly performed in the Cooperative Research Project Program of the Medical Institute of Bioregulation, Kyushu University. Publisher Copyright: © 2015 The Authors.

PY - 2015/9/22

Y1 - 2015/9/22

N2 - Rett syndrome (RTT) is a neurodevelopmental disorder caused by MECP2 mutations. Although emerging evidence suggests that MeCP2 deficiency is associated with dysregulation of mechanistic target of rapamycin (mTOR), which functions as a hub for various signaling pathways, the mechanism underlying this association and the molecular pathophysiology of RTT remain elusive. We show here that MeCP2 promotes the posttranscriptional processing of particular microRNAs (miRNAs) as a component of the microprocessor Drosha complex. Among the MeCP2-regulated miRNAs, we found that miR-199a positively controls mTOR signaling by targeting inhibitors for mTOR signaling. miR-199a and its targets have opposite effects on mTOR activity, ameliorating and inducing RTT neuronal phenotypes, respectively. Furthermore, genetic deletion of miR-199a-2 led to a reduction of mTOR activity in the brain and recapitulated numerous RTT phenotypes in mice. Together, these findings establish miR-199a as a critical downstream target of MeCP2 in RTT pathogenesis by linking MeCP2 with mTOR signaling.

AB - Rett syndrome (RTT) is a neurodevelopmental disorder caused by MECP2 mutations. Although emerging evidence suggests that MeCP2 deficiency is associated with dysregulation of mechanistic target of rapamycin (mTOR), which functions as a hub for various signaling pathways, the mechanism underlying this association and the molecular pathophysiology of RTT remain elusive. We show here that MeCP2 promotes the posttranscriptional processing of particular microRNAs (miRNAs) as a component of the microprocessor Drosha complex. Among the MeCP2-regulated miRNAs, we found that miR-199a positively controls mTOR signaling by targeting inhibitors for mTOR signaling. miR-199a and its targets have opposite effects on mTOR activity, ameliorating and inducing RTT neuronal phenotypes, respectively. Furthermore, genetic deletion of miR-199a-2 led to a reduction of mTOR activity in the brain and recapitulated numerous RTT phenotypes in mice. Together, these findings establish miR-199a as a critical downstream target of MeCP2 in RTT pathogenesis by linking MeCP2 with mTOR signaling.

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MiR-199a Links MeCP2 with mTOR Signaling and Its Dysregulation Leads to Rett Syndrome Phenotypes

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