Increased L1 retrotransposition in the neuronal genome in schizophrenia

Miki Bundo; Manabu Toyoshima; Yohei Okada; Wado Akamatsu; Junko Ueda; Taeko Nemoto-Miyauchi; Fumiko Sunaga; Michihiro Toritsuka; Daisuke Ikawa; Akiyoshi Kakita; Motoichiro Kato; Kiyoto Kasai; Toshifumi Kishimoto; Hiroyuki Nawa; Hideyuki Okano; Takeo Yoshikawa; Tadafumi Kato; Kazuya Iwamoto

doi:10.1016/j.neuron.2013.10.053

Increased L1 retrotransposition in the neuronal genome in schizophrenia

Miki Bundo, Manabu Toyoshima, Yohei Okada, Wado Akamatsu, Junko Ueda, Taeko Nemoto-Miyauchi, Fumiko Sunaga, Michihiro Toritsuka, Daisuke Ikawa, Akiyoshi Kakita, Motoichiro Kato, Kiyoto Kasai, Toshifumi Kishimoto, Hiroyuki Nawa, Hideyuki Okano, Takeo Yoshikawa, Tadafumi Kato, Kazuya Iwamoto

生理学

研究成果: Article › 査読

242 被引用数 (Scopus)

抄録

Recent studies indicate that long interspersed nuclear element-1 (L1) are mobilized in the genome of human neural progenitor cells and enhanced in Rett syndrome and ataxia telangiectasia. However, whether aberrant L1 retrotransposition occurs in mental disorders is unknown. Here, we report high L1 copy number in schizophrenia. Increased L1 was demonstrated in neurons from prefrontal cortex of patients and in induced pluripotent stem (iPS) cell-derived neurons containing 22q11 deletions. Whole-genome sequencing revealed brain-specific L1 insertion in patients localized preferentially to synapse- and schizophrenia-related genes. To study the mechanism of L1 transposition, we examined perinatal environmental risk factors for schizophrenia in animal models and observed an increased L1 copy number after immune activation by poly-I:C or epidermal growth factor. These findings suggest that hyperactive retrotransposition of L1 in neurons triggered by environmental and/or genetic risk factors may contribute to the susceptibility and pathophysiology of schizophrenia.

本文言語	English
ページ（範囲）	306-313
ページ数	8
ジャーナル	Neuron
巻	81
号	2
DOI	https://doi.org/10.1016/j.neuron.2013.10.053
出版ステータス	Published - 2014 1月 22

ASJC Scopus subject areas

神経科学（全般）

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10.1016/j.neuron.2013.10.053

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Bundo, M., Toyoshima, M., Okada, Y., Akamatsu, W., Ueda, J., Nemoto-Miyauchi, T., Sunaga, F., Toritsuka, M., Ikawa, D., Kakita, A., Kato, M., Kasai, K., Kishimoto, T., Nawa, H., Okano, H., Yoshikawa, T., Kato, T., & Iwamoto, K. (2014). Increased L1 retrotransposition in the neuronal genome in schizophrenia. Neuron, 81(2), 306-313. https://doi.org/10.1016/j.neuron.2013.10.053

Bundo, M, Toyoshima, M, Okada, Y, Akamatsu, W, Ueda, J, Nemoto-Miyauchi, T, Sunaga, F, Toritsuka, M, Ikawa, D, Kakita, A, Kato, M, Kasai, K, Kishimoto, T, Nawa, H, Okano, H, Yoshikawa, T, Kato, T & Iwamoto, K 2014, 'Increased L1 retrotransposition in the neuronal genome in schizophrenia', Neuron, vol. 81, no. 2, pp. 306-313. https://doi.org/10.1016/j.neuron.2013.10.053

@article{8770b79a1e5a423186b7412f0f8442a8,

title = "Increased L1 retrotransposition in the neuronal genome in schizophrenia",

abstract = "Recent studies indicate that long interspersed nuclear element-1 (L1) are mobilized in the genome of human neural progenitor cells and enhanced in Rett syndrome and ataxia telangiectasia. However, whether aberrant L1 retrotransposition occurs in mental disorders is unknown. Here, we report high L1 copy number in schizophrenia. Increased L1 was demonstrated in neurons from prefrontal cortex of patients and in induced pluripotent stem (iPS) cell-derived neurons containing 22q11 deletions. Whole-genome sequencing revealed brain-specific L1 insertion in patients localized preferentially to synapse- and schizophrenia-related genes. To study the mechanism of L1 transposition, we examined perinatal environmental risk factors for schizophrenia in animal models and observed an increased L1 copy number after immune activation by poly-I:C or epidermal growth factor. These findings suggest that hyperactive retrotransposition of L1 in neurons triggered by environmental and/or genetic risk factors may contribute to the susceptibility and pathophysiology of schizophrenia.",

author = "Miki Bundo and Manabu Toyoshima and Yohei Okada and Wado Akamatsu and Junko Ueda and Taeko Nemoto-Miyauchi and Fumiko Sunaga and Michihiro Toritsuka and Daisuke Ikawa and Akiyoshi Kakita and Motoichiro Kato and Kiyoto Kasai and Toshifumi Kishimoto and Hiroyuki Nawa and Hideyuki Okano and Takeo Yoshikawa and Tadafumi Kato and Kazuya Iwamoto",

note = "Funding Information: This work was supported in part by the Grant-in-Aid for Scientific Research on Innovative Areas (Unraveling the microendophenotypes of psychiatric disorders at the molecular, cellular, and circuit levels) from the Ministry of Education, Culture, Sports, Science and Technology (MEXT) to T.Y., H.N., T.K., and K.I., and a Grant-in-Aid from Ministry of Health, Labour and Welfare to T.K. This work was also supported by JST, CREST to T.K. and by JST, PRESTO to K.I. This work was also supported in part by Leading Project for Realization of Regenerative Medicine from MEXT and “Funding Program for World-Leading Innovative R&D on Science and Technology” to H.O., and by the “Development of biomarker candidates for social behavior” carried out under the Strategic Research Program for Brain Sciences from MEXT to T.Y. and K.K. This work was also supported in part by the Collaborative Research Project of the Brain Research Institute, Niigata University . Postmortem samples were donated by the Stanley Medical Research Institute, courtesy of Drs. Michael B. Knable, E. Fuller Torrey, Maree J. Webster, and Robert H. Yolken. We thank Tomoko Toyota and Atsuko Komori-Kokubo at RIKEN BSI for their technical assistance. We also thank Kenji Ohtawa at Research Resources Center at the RIKEN BSI for the cell-sorting analysis. M.B., F.S., and K.I. belong to the Department of Molecular Psychiatry, which is endowed by Dainippon Sumitomo Pharma and Yoshitomiyakuhin. H.O. is a scientific consultant for San Bio, Eisai, and Daiichi Sankyo. T.K. received a grant from Takeda Pharmaceutical . These companies had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. ",

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doi = "10.1016/j.neuron.2013.10.053",

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AU - Bundo, Miki

AU - Toyoshima, Manabu

AU - Okada, Yohei

AU - Akamatsu, Wado

AU - Ueda, Junko

AU - Nemoto-Miyauchi, Taeko

AU - Sunaga, Fumiko

AU - Toritsuka, Michihiro

AU - Ikawa, Daisuke

AU - Kakita, Akiyoshi

AU - Kato, Motoichiro

AU - Kasai, Kiyoto

AU - Kishimoto, Toshifumi

AU - Nawa, Hiroyuki

AU - Okano, Hideyuki

AU - Yoshikawa, Takeo

AU - Kato, Tadafumi

AU - Iwamoto, Kazuya

N1 - Funding Information: This work was supported in part by the Grant-in-Aid for Scientific Research on Innovative Areas (Unraveling the microendophenotypes of psychiatric disorders at the molecular, cellular, and circuit levels) from the Ministry of Education, Culture, Sports, Science and Technology (MEXT) to T.Y., H.N., T.K., and K.I., and a Grant-in-Aid from Ministry of Health, Labour and Welfare to T.K. This work was also supported by JST, CREST to T.K. and by JST, PRESTO to K.I. This work was also supported in part by Leading Project for Realization of Regenerative Medicine from MEXT and “Funding Program for World-Leading Innovative R&D on Science and Technology” to H.O., and by the “Development of biomarker candidates for social behavior” carried out under the Strategic Research Program for Brain Sciences from MEXT to T.Y. and K.K. This work was also supported in part by the Collaborative Research Project of the Brain Research Institute, Niigata University . Postmortem samples were donated by the Stanley Medical Research Institute, courtesy of Drs. Michael B. Knable, E. Fuller Torrey, Maree J. Webster, and Robert H. Yolken. We thank Tomoko Toyota and Atsuko Komori-Kokubo at RIKEN BSI for their technical assistance. We also thank Kenji Ohtawa at Research Resources Center at the RIKEN BSI for the cell-sorting analysis. M.B., F.S., and K.I. belong to the Department of Molecular Psychiatry, which is endowed by Dainippon Sumitomo Pharma and Yoshitomiyakuhin. H.O. is a scientific consultant for San Bio, Eisai, and Daiichi Sankyo. T.K. received a grant from Takeda Pharmaceutical . These companies had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.

PY - 2014/1/22

Y1 - 2014/1/22

N2 - Recent studies indicate that long interspersed nuclear element-1 (L1) are mobilized in the genome of human neural progenitor cells and enhanced in Rett syndrome and ataxia telangiectasia. However, whether aberrant L1 retrotransposition occurs in mental disorders is unknown. Here, we report high L1 copy number in schizophrenia. Increased L1 was demonstrated in neurons from prefrontal cortex of patients and in induced pluripotent stem (iPS) cell-derived neurons containing 22q11 deletions. Whole-genome sequencing revealed brain-specific L1 insertion in patients localized preferentially to synapse- and schizophrenia-related genes. To study the mechanism of L1 transposition, we examined perinatal environmental risk factors for schizophrenia in animal models and observed an increased L1 copy number after immune activation by poly-I:C or epidermal growth factor. These findings suggest that hyperactive retrotransposition of L1 in neurons triggered by environmental and/or genetic risk factors may contribute to the susceptibility and pathophysiology of schizophrenia.

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Increased L1 retrotransposition in the neuronal genome in schizophrenia

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