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A role for the Ras signalling pathway in synaptic transmission and long-term memory

Author

Listed:
  • Riccardo Brambilla

    (European Molecular Biology Laboratory
    DIBIT, Istituto Scientifico San Raffaele)

  • Nerina Gnesutta

    (Universita' di Milano)

  • Liliana Minichiello

    (European Molecular Biology Laboratory)

  • Gail White

    (Physiology Unit, School of Molecular and Medical Biosciences, University of Wales)

  • Alistair J. Roylance

    (Centre for Genome Research, University of Edinburgh)

  • Caroline E. Herron

    (Centre for Genome Research, University of Edinburgh
    Centre for Neuroscience, University of Edinburgh)

  • Mark Ramsey

    (Centre for Neuroscience, University of Edinburgh)

  • David P. Wolfer

    (Anatomisches Institut, Universität Zürich)

  • Vincenzo Cestari

    (Istituto di Psicobiologia e Psicofarmacologia del Consiglio Nazionale delle Ricerche)

  • Clelia Rossi-Arnaud

    (Universita' di Roma La Sapienza)

  • Seth G. N. Grant

    (Centre for Genome Research, University of Edinburgh
    Centre for Neuroscience, University of Edinburgh)

  • Paul F. Chapman

    (Physiology Unit, School of Molecular and Medical Biosciences, University of Wales)

  • Hans-Peter Lipp

    (Anatomisches Institut, Universität Zürich)

  • Emmapaola Sturani

    (Universita' di Milano)

  • Rdiger Klein

    (European Molecular Biology Laboratory)

Abstract

Members of the Ras subfamily of small guanine-nucleotide-binding proteins are essential for controlling normal and malignant cell proliferation as well as cell differentiation1. The neuronal-specific guanine-nucleotide-exchange factor, Ras-GRF/CDC25Mm (refs 2,3,4), induces Ras signalling in response to Ca2+ influx5 and activation of G-protein-coupled receptors in vitro6, suggesting that it plays a role in neurotransmission and plasticity in vivo7. Here we report that mice lacking Ras-GRF are impaired in the process of memory consolidation, as revealed by emotional conditioning tasks that require the function of the amygdala; learning and short-term memory are intact. Electrophysiological measurements in the basolateral amygdala reveal that long-term plasticity is abnormal in mutant mice. In contrast, Ras-GRF mutants do not reveal major deficits in spatial learning tasks such as the Morris water maze, a test that requires hippocampal function. Consistent with apparently normal hippocampal functions, Ras-GRF mutants show normal NMDA (N-methyl-D-aspartate) receptor-dependent long-term potentiation in this structure. These results implicate Ras-GRF signalling via the Ras/MAP kinase pathway in synaptic events leading to formation of long-term memories.

Suggested Citation

  • Riccardo Brambilla & Nerina Gnesutta & Liliana Minichiello & Gail White & Alistair J. Roylance & Caroline E. Herron & Mark Ramsey & David P. Wolfer & Vincenzo Cestari & Clelia Rossi-Arnaud & Seth G. N, 1997. "A role for the Ras signalling pathway in synaptic transmission and long-term memory," Nature, Nature, vol. 390(6657), pages 281-286, November.
  • Handle: RePEc:nat:nature:v:390:y:1997:i:6657:d:10.1038_36849
    DOI: 10.1038/36849
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    1. Yee-Ling Wong & Pirro Hysi & Gemmy Cheung & Milly Tedja & Quan V Hoang & Stuart W J Tompson & Kristina N Whisenhunt & Virginie Verhoeven & Wanting Zhao & Moritz Hess & Chee-Wai Wong & Annette Kifley &, 2019. "Genetic variants linked to myopic macular degeneration in persons with high myopia: CREAM Consortium," PLOS ONE, Public Library of Science, vol. 14(8), pages 1-16, August.

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