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eIF2α controls memory consolidation via excitatory and somatostatin neurons

Author

Listed:
  • Vijendra Sharma

    (McGill University
    McGill University)

  • Rapita Sood

    (McGill University
    McGill University)

  • Abdessattar Khlaifia

    (University of Montréal)

  • Mohammad Javad Eslamizade

    (McGill University
    McGill University
    University of Montréal)

  • Tzu-Yu Hung

    (McGill University
    McGill University)

  • Danning Lou

    (McGill University
    McGill University)

  • Azam Asgarihafshejani

    (University of Montréal)

  • Maya Lalzar

    (University of Haifa)

  • Stephen J. Kiniry

    (University College Cork)

  • Matthew P. Stokes

    (Proteomics Division, Cell Signaling Technology)

  • Noah Cohen

    (McGill University
    McGill University)

  • Alissa J. Nelson

    (Proteomics Division, Cell Signaling Technology)

  • Kathryn Abell

    (Proteomics Division, Cell Signaling Technology)

  • Anthony P. Possemato

    (Proteomics Division, Cell Signaling Technology)

  • Shunit Gal-Ben-Ari

    (University of Haifa)

  • Vinh T. Truong

    (McGill University
    McGill University)

  • Peng Wang

    (McGill University
    McGill University)

  • Adonis Yiannakas

    (University of Haifa)

  • Fatemeh Saffarzadeh

    (University of Montréal)

  • A. Claudio Cuello

    (McGill University)

  • Karim Nader

    (McGill University)

  • Randal J. Kaufman

    (Sanford-Burnham-Prebys Medical Discovery Institute)

  • Mauro Costa-Mattioli

    (Baylor College of Medicine)

  • Pavel V. Baranov

    (University College Cork
    Shemyakin and Ovchinnikov Institute of Bioorganic Chemistry, RAS)

  • Albert Quintana

    (Universitat Autònoma de Barcelona
    Universitat Autònoma de Barcelona)

  • Elisenda Sanz

    (Universitat Autònoma de Barcelona
    Universitat Autònoma de Barcelona)

  • Arkady Khoutorsky

    (McGill University
    McGill University)

  • Jean-Claude Lacaille

    (University of Montréal
    University of Montréal)

  • Kobi Rosenblum

    (University of Haifa
    University of Haifa)

  • Nahum Sonenberg

    (McGill University
    McGill University)

Abstract

An important tenet of learning and memory is the notion of a molecular switch that promotes the formation of long-term memory1–4. The regulation of proteostasis is a critical and rate-limiting step in the consolidation of new memories5–10. One of the most effective and prevalent ways to enhance memory is by regulating the synthesis of proteins controlled by the translation initiation factor eIF211. Phosphorylation of the α-subunit of eIF2 (p-eIF2α), the central component of the integrated stress response (ISR), impairs long-term memory formation in rodents and birds11–13. By contrast, inhibiting the ISR by mutating the eIF2α phosphorylation site, genetically11 and pharmacologically inhibiting the ISR kinases14–17, or mimicking reduced p-eIF2α with the ISR inhibitor ISRIB11, enhances long-term memory in health and disease18. Here we used molecular genetics to dissect the neuronal circuits by which the ISR gates cognitive processing. We found that learning reduces eIF2α phosphorylation in hippocampal excitatory neurons and a subset of hippocampal inhibitory neurons (those that express somatostatin, but not parvalbumin). Moreover, ablation of p-eIF2α in either excitatory or somatostatin-expressing (but not parvalbumin-expressing) inhibitory neurons increased general mRNA translation, bolstered synaptic plasticity and enhanced long-term memory. Thus, eIF2α-dependent mRNA translation controls memory consolidation via autonomous mechanisms in excitatory and somatostatin-expressing inhibitory neurons.

Suggested Citation

  • Vijendra Sharma & Rapita Sood & Abdessattar Khlaifia & Mohammad Javad Eslamizade & Tzu-Yu Hung & Danning Lou & Azam Asgarihafshejani & Maya Lalzar & Stephen J. Kiniry & Matthew P. Stokes & Noah Cohen , 2020. "eIF2α controls memory consolidation via excitatory and somatostatin neurons," Nature, Nature, vol. 586(7829), pages 412-416, October.
  • Handle: RePEc:nat:nature:v:586:y:2020:i:7829:d:10.1038_s41586-020-2805-8
    DOI: 10.1038/s41586-020-2805-8
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    Cited by:

    1. G. Torromino & V. Loffredo & D. Cavezza & G. Sonsini & F. Esposito & A. H. Crevenna & M. Gioffrè & M. De Risi & A. Treves & M. Griguoli & E. De Leonibus, 2022. "Thalamo-hippocampal pathway regulates incidental memory capacity in mice," Nature Communications, Nature, vol. 13(1), pages 1-14, December.

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