Rab GTPases-dependent endocytic pathways regulate neuronal migration and maturation through N-cadherin trafficking

Takeshi Kawauchi; Katsutoshi Sekine; Mima Shikanai; Kaori Chihama; Kenji Tomita; Ken ichiro Kubo; Kazunori Nakajima; Yo ichi Nabeshima; Mikio Hoshino

doi:10.1016/j.neuron.2010.07.007

Rab GTPases-dependent endocytic pathways regulate neuronal migration and maturation through N-cadherin trafficking

Takeshi Kawauchi^*, Katsutoshi Sekine, Mima Shikanai, Kaori Chihama, Kenji Tomita, Ken ichiro Kubo, Kazunori Nakajima, Yo ichi Nabeshima, Mikio Hoshino

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

251 Citations (Scopus)

Abstract

Although membrane trafficking pathways are involved in basic cellular functions, the evolutionally expanded number of their related family proteins suggests additional roles for membrane trafficking in higher organisms. Here, we show that several Rab-dependent trafficking pathways differentially participate in neuronal migration, an essential step for the formation of the mammalian-specific six-layered brain structure. In vivo electroporation-mediated suppression of Rab5 or dynamin to block endocytosis caused a severe neuronal migration defect in mouse cerebral cortex. Among many downstream endocytic pathways, suppression of Rab11-dependent recycling pathways exhibited a similar migration disorder, whereas inhibition of Rab7-dependent lysosomal degradation pathways affected only the final phase of neuronal migration and dendrite morphology. Inhibition of Rab5 or Rab11 perturbed the trafficking of N-cadherin, whose suppression also disturbed neuronal migration. Taken together, our findings reveal physiological roles of endocytic pathways, each of which has specific functions in distinct steps of neuronal migration and maturation during mammalian brain formation.

Original language	English
Pages (from-to)	588-602
Number of pages	15
Journal	Neuron
Volume	67
Issue number	4
DOIs	https://doi.org/10.1016/j.neuron.2010.07.007
Publication status	Published - 2010 Aug
Externally published	Yes

ASJC Scopus subject areas

Neuroscience(all)

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10.1016/j.neuron.2010.07.007

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@article{f97b9791d48c41c19f917912dfd28871,

title = "Rab GTPases-dependent endocytic pathways regulate neuronal migration and maturation through N-cadherin trafficking",

abstract = "Although membrane trafficking pathways are involved in basic cellular functions, the evolutionally expanded number of their related family proteins suggests additional roles for membrane trafficking in higher organisms. Here, we show that several Rab-dependent trafficking pathways differentially participate in neuronal migration, an essential step for the formation of the mammalian-specific six-layered brain structure. In vivo electroporation-mediated suppression of Rab5 or dynamin to block endocytosis caused a severe neuronal migration defect in mouse cerebral cortex. Among many downstream endocytic pathways, suppression of Rab11-dependent recycling pathways exhibited a similar migration disorder, whereas inhibition of Rab7-dependent lysosomal degradation pathways affected only the final phase of neuronal migration and dendrite morphology. Inhibition of Rab5 or Rab11 perturbed the trafficking of N-cadherin, whose suppression also disturbed neuronal migration. Taken together, our findings reveal physiological roles of endocytic pathways, each of which has specific functions in distinct steps of neuronal migration and maturation during mammalian brain formation.",

author = "Takeshi Kawauchi and Katsutoshi Sekine and Mima Shikanai and Kaori Chihama and Kenji Tomita and Kubo, {Ken ichiro} and Kazunori Nakajima and Nabeshima, {Yo ichi} and Mikio Hoshino",

note = "Funding Information: We thank T. Baba, C. Bucci, S. Hirai, R. L. Huganir, S. Kanda, B. J. Knoll, D. Manor, M. McCaffrey, F. D. Miller, J. Miyazaki, M. Ozawa, R. E. Pagano, K. Takei, K. Tanabe, and D. L. Turner for providing plasmids, Kaori Kawauchi for a part of statistical analyses, and Ruth T. Yu and Akira Sakakibara for helpful comments. We also thank the Core Instrumentation Facility, Keio University School of Medicine for help with Leica SP5 confocal microscopy, LAS4000mini, FACS and ABI DNA sequencer. This work was supported by Grants-in-Aid from the Ministry of Education, Culture, Sports, and Science and Technology, Japan (#21113524 to T.K., #19670002 to M.H., and #22240041 to K.N.), and by grants from the JST PRESTO program, Takeda Science Foundation and GCOE. Author contributions; T.K. conceived the study and designed and performed experiments. K.S., M.S., and K.C. performed experiments. K.T. partly performed N-cadherin knockdown. K.K. constructed a part of N-cadherin vectors. Y.N., M.H., K.N., and T.K. administrated the experimental environments. T.K. jointly wrote the paper with M.H. ",

year = "2010",

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doi = "10.1016/j.neuron.2010.07.007",

language = "English",

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journal = "Neuron",

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T1 - Rab GTPases-dependent endocytic pathways regulate neuronal migration and maturation through N-cadherin trafficking

AU - Kawauchi, Takeshi

AU - Sekine, Katsutoshi

AU - Shikanai, Mima

AU - Chihama, Kaori

AU - Tomita, Kenji

AU - Kubo, Ken ichiro

AU - Nakajima, Kazunori

AU - Nabeshima, Yo ichi

AU - Hoshino, Mikio

N1 - Funding Information: We thank T. Baba, C. Bucci, S. Hirai, R. L. Huganir, S. Kanda, B. J. Knoll, D. Manor, M. McCaffrey, F. D. Miller, J. Miyazaki, M. Ozawa, R. E. Pagano, K. Takei, K. Tanabe, and D. L. Turner for providing plasmids, Kaori Kawauchi for a part of statistical analyses, and Ruth T. Yu and Akira Sakakibara for helpful comments. We also thank the Core Instrumentation Facility, Keio University School of Medicine for help with Leica SP5 confocal microscopy, LAS4000mini, FACS and ABI DNA sequencer. This work was supported by Grants-in-Aid from the Ministry of Education, Culture, Sports, and Science and Technology, Japan (#21113524 to T.K., #19670002 to M.H., and #22240041 to K.N.), and by grants from the JST PRESTO program, Takeda Science Foundation and GCOE. Author contributions; T.K. conceived the study and designed and performed experiments. K.S., M.S., and K.C. performed experiments. K.T. partly performed N-cadherin knockdown. K.K. constructed a part of N-cadherin vectors. Y.N., M.H., K.N., and T.K. administrated the experimental environments. T.K. jointly wrote the paper with M.H.

PY - 2010/8

Y1 - 2010/8

N2 - Although membrane trafficking pathways are involved in basic cellular functions, the evolutionally expanded number of their related family proteins suggests additional roles for membrane trafficking in higher organisms. Here, we show that several Rab-dependent trafficking pathways differentially participate in neuronal migration, an essential step for the formation of the mammalian-specific six-layered brain structure. In vivo electroporation-mediated suppression of Rab5 or dynamin to block endocytosis caused a severe neuronal migration defect in mouse cerebral cortex. Among many downstream endocytic pathways, suppression of Rab11-dependent recycling pathways exhibited a similar migration disorder, whereas inhibition of Rab7-dependent lysosomal degradation pathways affected only the final phase of neuronal migration and dendrite morphology. Inhibition of Rab5 or Rab11 perturbed the trafficking of N-cadherin, whose suppression also disturbed neuronal migration. Taken together, our findings reveal physiological roles of endocytic pathways, each of which has specific functions in distinct steps of neuronal migration and maturation during mammalian brain formation.

AB - Although membrane trafficking pathways are involved in basic cellular functions, the evolutionally expanded number of their related family proteins suggests additional roles for membrane trafficking in higher organisms. Here, we show that several Rab-dependent trafficking pathways differentially participate in neuronal migration, an essential step for the formation of the mammalian-specific six-layered brain structure. In vivo electroporation-mediated suppression of Rab5 or dynamin to block endocytosis caused a severe neuronal migration defect in mouse cerebral cortex. Among many downstream endocytic pathways, suppression of Rab11-dependent recycling pathways exhibited a similar migration disorder, whereas inhibition of Rab7-dependent lysosomal degradation pathways affected only the final phase of neuronal migration and dendrite morphology. Inhibition of Rab5 or Rab11 perturbed the trafficking of N-cadherin, whose suppression also disturbed neuronal migration. Taken together, our findings reveal physiological roles of endocytic pathways, each of which has specific functions in distinct steps of neuronal migration and maturation during mammalian brain formation.

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JO - Neuron

JF - Neuron

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ER -

Rab GTPases-dependent endocytic pathways regulate neuronal migration and maturation through N-cadherin trafficking

Abstract

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