The transcriptional repressor RP58 is crucial for cell-division patterning and neuronal survival in the developing cortex

Haruo Okado; Chiaki Ohtaka-Maruyama; Yoshinobu Sugitani; Yuko Fukuda; Reiko Ishida; Shinobu Hirai; Akiko Miwa; Akiyo Takahashi; Katsunori Aoki; Keiji Mochida; Osamu Suzuki; Takao Honda; Kazunori Nakajima; Masaharu Ogawa; Toshio Terashima; Junichiro Matsuda; Hitoshi Kawano; Masataka Kasai

doi:10.1016/j.ydbio.2009.04.030

The transcriptional repressor RP58 is crucial for cell-division patterning and neuronal survival in the developing cortex

Haruo Okado, Chiaki Ohtaka-Maruyama, Yoshinobu Sugitani, Yuko Fukuda, Reiko Ishida, Shinobu Hirai, Akiko Miwa, Akiyo Takahashi, Katsunori Aoki, Keiji Mochida, Osamu Suzuki, Takao Honda, Kazunori Nakajima, Masaharu Ogawa, Toshio Terashima, Junichiro Matsuda, Hitoshi Kawano, Masataka Kasai

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研究成果: Article › 査読

47 被引用数 (Scopus)

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The neocortex and the hippocampus comprise several specific layers containing distinct neurons that originate from progenitors at specific development times, under the control of an adequate cell-division patterning mechanism. Although many molecules are known to regulate this cell-division patterning process, its details are not well understood. Here, we show that, in the developing cerebral cortex, the RP58 transcription repressor protein was expressed both in postmitotic glutamatergic projection neurons and in their progenitor cells, but not in GABAergic interneurons. Targeted deletion of the RP58 gene led to dysplasia of the neocortex and of the hippocampus, reduction of the number of mature cortical neurons, and defects of laminar organization, which reflect abnormal neuronal migration within the cortical plate. We demonstrate an impairment of the cell-division patterning during the late embryonic stage and an enhancement of apoptosis of the postmitotic neurons in the RP58-deficient cortex. These results suggest that RP58 controls cell division of progenitor cells and regulates the survival of postmitotic cortical neurons.

本文言語	English
ページ（範囲）	140-151
ページ数	12
ジャーナル	Developmental Biology
巻	331
号	2
DOI	https://doi.org/10.1016/j.ydbio.2009.04.030
出版ステータス	Published - 2009 7月 15

ASJC Scopus subject areas

分子生物学
発生生物学
細胞生物学

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10.1016/j.ydbio.2009.04.030

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Okado, H., Ohtaka-Maruyama, C., Sugitani, Y., Fukuda, Y., Ishida, R., Hirai, S., Miwa, A., Takahashi, A., Aoki, K., Mochida, K., Suzuki, O., Honda, T., Nakajima, K., Ogawa, M., Terashima, T., Matsuda, J., Kawano, H., & Kasai, M. (2009). The transcriptional repressor RP58 is crucial for cell-division patterning and neuronal survival in the developing cortex. Developmental Biology, 331(2), 140-151. https://doi.org/10.1016/j.ydbio.2009.04.030

Okado, H, Ohtaka-Maruyama, C, Sugitani, Y, Fukuda, Y, Ishida, R, Hirai, S, Miwa, A, Takahashi, A, Aoki, K, Mochida, K, Suzuki, O, Honda, T, Nakajima, K, Ogawa, M, Terashima, T, Matsuda, J, Kawano, H & Kasai, M 2009, 'The transcriptional repressor RP58 is crucial for cell-division patterning and neuronal survival in the developing cortex', Developmental Biology, vol. 331, no. 2, pp. 140-151. https://doi.org/10.1016/j.ydbio.2009.04.030

@article{222ff6f5b97d4fb0a25110ea74f00123,

title = "The transcriptional repressor RP58 is crucial for cell-division patterning and neuronal survival in the developing cortex",

abstract = "The neocortex and the hippocampus comprise several specific layers containing distinct neurons that originate from progenitors at specific development times, under the control of an adequate cell-division patterning mechanism. Although many molecules are known to regulate this cell-division patterning process, its details are not well understood. Here, we show that, in the developing cerebral cortex, the RP58 transcription repressor protein was expressed both in postmitotic glutamatergic projection neurons and in their progenitor cells, but not in GABAergic interneurons. Targeted deletion of the RP58 gene led to dysplasia of the neocortex and of the hippocampus, reduction of the number of mature cortical neurons, and defects of laminar organization, which reflect abnormal neuronal migration within the cortical plate. We demonstrate an impairment of the cell-division patterning during the late embryonic stage and an enhancement of apoptosis of the postmitotic neurons in the RP58-deficient cortex. These results suggest that RP58 controls cell division of progenitor cells and regulates the survival of postmitotic cortical neurons.",

keywords = "Apoptosis, Cell-cycle exit, Cerebral cortex, Progenitor cell, RP58, Transcriptional repressor",

author = "Haruo Okado and Chiaki Ohtaka-Maruyama and Yoshinobu Sugitani and Yuko Fukuda and Reiko Ishida and Shinobu Hirai and Akiko Miwa and Akiyo Takahashi and Katsunori Aoki and Keiji Mochida and Osamu Suzuki and Takao Honda and Kazunori Nakajima and Masaharu Ogawa and Toshio Terashima and Junichiro Matsuda and Hitoshi Kawano and Masataka Kasai",

note = "Funding Information: We thank Drs. Koki Kawamura, Makoto Hashimoto, Minoru Saitoe, Junjiro Horiuchi (Tokyo Metropolitan Institute for Neuroscience (TMIN)), Douglas E. Vetter (Tufts University School of Medicine), and Mitsuharu Hattori (Nagoya City University) for critical suggestions. We also thank Dr. Kazuaki Yoshikawa (Osaka University) for the guinea pig anti-Dlx2 antibody and Dr. David Anderson (California Institute of Technology) for the mouse anti-Neurogenin2 antibody. We thank Drs. Yoshinobu Sugitani and Tetsuo Noda (JFCR-Cancer Institute) for providing the mouse CTGF , mouse Tailless , mouse Tbr1 , and mouse SorLA cDNAs used to prepare the probes for RNA in situ hybridization, as well as Dr. Thomas M. Jessell (Columbia University Medical Center) for mouse ER81 , Dr. Susan K. McConnell (Stanford University) for mouse ROR β, Dr. Victor Tarabykin (Max Planck Institute of Biophysical Chemistry) for Svet1 , Dr. Shinichi Aizawa (RIKEN Kobe) for NT3 , Dr. Greg E. Lemke (Salk Institute) for SCIP , Dr. Jim Boulter (UCLA Brain Research and Molecular Biology Institutes) for KA1 , and Dr. Francois Guillemot (NIMR) for HES5 cDNAs. We also thank Ms. Yasuko Kishimoto (Histology Center, TMIN) for her technical assistance. These studies were supported by a grant-in-aid from the Ministry of Science, Education and Culture to H. O. and by Human Science Research Funds and the Budget for Nuclear Research of the MEXT, awarded to M. K. ",

year = "2009",

month = jul,

day = "15",

doi = "10.1016/j.ydbio.2009.04.030",

language = "English",

volume = "331",

pages = "140--151",

journal = "Developmental Biology",

issn = "0012-1606",

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T1 - The transcriptional repressor RP58 is crucial for cell-division patterning and neuronal survival in the developing cortex

AU - Okado, Haruo

AU - Ohtaka-Maruyama, Chiaki

AU - Sugitani, Yoshinobu

AU - Fukuda, Yuko

AU - Ishida, Reiko

AU - Hirai, Shinobu

AU - Miwa, Akiko

AU - Takahashi, Akiyo

AU - Aoki, Katsunori

AU - Mochida, Keiji

AU - Suzuki, Osamu

AU - Honda, Takao

AU - Nakajima, Kazunori

AU - Ogawa, Masaharu

AU - Terashima, Toshio

AU - Matsuda, Junichiro

AU - Kawano, Hitoshi

AU - Kasai, Masataka

N1 - Funding Information: We thank Drs. Koki Kawamura, Makoto Hashimoto, Minoru Saitoe, Junjiro Horiuchi (Tokyo Metropolitan Institute for Neuroscience (TMIN)), Douglas E. Vetter (Tufts University School of Medicine), and Mitsuharu Hattori (Nagoya City University) for critical suggestions. We also thank Dr. Kazuaki Yoshikawa (Osaka University) for the guinea pig anti-Dlx2 antibody and Dr. David Anderson (California Institute of Technology) for the mouse anti-Neurogenin2 antibody. We thank Drs. Yoshinobu Sugitani and Tetsuo Noda (JFCR-Cancer Institute) for providing the mouse CTGF , mouse Tailless , mouse Tbr1 , and mouse SorLA cDNAs used to prepare the probes for RNA in situ hybridization, as well as Dr. Thomas M. Jessell (Columbia University Medical Center) for mouse ER81 , Dr. Susan K. McConnell (Stanford University) for mouse ROR β, Dr. Victor Tarabykin (Max Planck Institute of Biophysical Chemistry) for Svet1 , Dr. Shinichi Aizawa (RIKEN Kobe) for NT3 , Dr. Greg E. Lemke (Salk Institute) for SCIP , Dr. Jim Boulter (UCLA Brain Research and Molecular Biology Institutes) for KA1 , and Dr. Francois Guillemot (NIMR) for HES5 cDNAs. We also thank Ms. Yasuko Kishimoto (Histology Center, TMIN) for her technical assistance. These studies were supported by a grant-in-aid from the Ministry of Science, Education and Culture to H. O. and by Human Science Research Funds and the Budget for Nuclear Research of the MEXT, awarded to M. K.

PY - 2009/7/15

Y1 - 2009/7/15

N2 - The neocortex and the hippocampus comprise several specific layers containing distinct neurons that originate from progenitors at specific development times, under the control of an adequate cell-division patterning mechanism. Although many molecules are known to regulate this cell-division patterning process, its details are not well understood. Here, we show that, in the developing cerebral cortex, the RP58 transcription repressor protein was expressed both in postmitotic glutamatergic projection neurons and in their progenitor cells, but not in GABAergic interneurons. Targeted deletion of the RP58 gene led to dysplasia of the neocortex and of the hippocampus, reduction of the number of mature cortical neurons, and defects of laminar organization, which reflect abnormal neuronal migration within the cortical plate. We demonstrate an impairment of the cell-division patterning during the late embryonic stage and an enhancement of apoptosis of the postmitotic neurons in the RP58-deficient cortex. These results suggest that RP58 controls cell division of progenitor cells and regulates the survival of postmitotic cortical neurons.

AB - The neocortex and the hippocampus comprise several specific layers containing distinct neurons that originate from progenitors at specific development times, under the control of an adequate cell-division patterning mechanism. Although many molecules are known to regulate this cell-division patterning process, its details are not well understood. Here, we show that, in the developing cerebral cortex, the RP58 transcription repressor protein was expressed both in postmitotic glutamatergic projection neurons and in their progenitor cells, but not in GABAergic interneurons. Targeted deletion of the RP58 gene led to dysplasia of the neocortex and of the hippocampus, reduction of the number of mature cortical neurons, and defects of laminar organization, which reflect abnormal neuronal migration within the cortical plate. We demonstrate an impairment of the cell-division patterning during the late embryonic stage and an enhancement of apoptosis of the postmitotic neurons in the RP58-deficient cortex. These results suggest that RP58 controls cell division of progenitor cells and regulates the survival of postmitotic cortical neurons.

KW - Apoptosis

KW - Cell-cycle exit

KW - Cerebral cortex

KW - Progenitor cell

KW - RP58

KW - Transcriptional repressor

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U2 - 10.1016/j.ydbio.2009.04.030

DO - 10.1016/j.ydbio.2009.04.030

M3 - Article

C2 - 19409883

AN - SCOPUS:67549091231

SN - 0012-1606

VL - 331

SP - 140

EP - 151

JO - Developmental Biology

JF - Developmental Biology

IS - 2

ER -

The transcriptional repressor RP58 is crucial for cell-division patterning and neuronal survival in the developing cortex

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