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Antidepressant actions of ketamine engage cell-specific translation via eIF4E

Author

Listed:
  • Argel Aguilar-Valles

    (McGill University
    Université de Montréal
    Carleton University)

  • Danilo De Gregorio

    (McGill University
    McGill University)

  • Edna Matta-Camacho

    (McGill University
    Carleton University)

  • Mohammad J. Eslamizade

    (McGill University
    Université de Montréal)

  • Abdessattar Khlaifia

    (Université de Montréal)

  • Agnieszka Skaleka

    (McGill University)

  • Martha Lopez-Canul

    (McGill University)

  • Angelica Torres-Berrio

    (Friedman Brain Institute, Icahn School of Medicine at Mount Sinai)

  • Sara Bermudez

    (McGill University)

  • Gareth M. Rurak

    (Carleton University)

  • Stephanie Simard

    (Carleton University)

  • Natalina Salmaso

    (Carleton University)

  • Gabriella Gobbi

    (McGill University)

  • Jean-Claude Lacaille

    (Université de Montréal)

  • Nahum Sonenberg

    (McGill University)

Abstract

Effective pharmacotherapy for major depressive disorder remains a major challenge, as more than 30% of patients are resistant to the first line of treatment (selective serotonin reuptake inhibitors)1. Sub-anaesthetic doses of ketamine, a non-competitive N-methyl-d-aspartate receptor antagonist2,3, provide rapid and long-lasting antidepressant effects in these patients4–6, but the molecular mechanism of these effects remains unclear7,8. Ketamine has been proposed to exert its antidepressant effects through its metabolite (2R,6R)-hydroxynorketamine ((2R,6R)-HNK)9. The antidepressant effects of ketamine and (2R,6R)-HNK in rodents require activation of the mTORC1 kinase10,11. mTORC1 controls various neuronal functions12, particularly through cap-dependent initiation of mRNA translation via the phosphorylation and inactivation of eukaryotic initiation factor 4E-binding proteins (4E-BPs)13. Here we show that 4E-BP1 and 4E-BP2 are key effectors of the antidepressant activity of ketamine and (2R,6R)-HNK, and that ketamine-induced hippocampal synaptic plasticity depends on 4E-BP2 and, to a lesser extent, 4E-BP1. It has been hypothesized that ketamine activates mTORC1–4E-BP signalling in pyramidal excitatory cells of the cortex8,14. To test this hypothesis, we studied the behavioural response to ketamine and (2R,6R)-HNK in mice lacking 4E-BPs in either excitatory or inhibitory neurons. The antidepressant activity of the drugs is mediated by 4E-BP2 in excitatory neurons, and 4E-BP1 and 4E-BP2 in inhibitory neurons. Notably, genetic deletion of 4E-BP2 in inhibitory neurons induced a reduction in baseline immobility in the forced swim test, mimicking an antidepressant effect. Deletion of 4E-BP2 specifically in inhibitory neurons also prevented the ketamine-induced increase in hippocampal excitatory neurotransmission, and this effect concurred with the inability of ketamine to induce a long-lasting decrease in inhibitory neurotransmission. Overall, our data show that 4E-BPs are central to the antidepressant activity of ketamine.

Suggested Citation

  • Argel Aguilar-Valles & Danilo De Gregorio & Edna Matta-Camacho & Mohammad J. Eslamizade & Abdessattar Khlaifia & Agnieszka Skaleka & Martha Lopez-Canul & Angelica Torres-Berrio & Sara Bermudez & Garet, 2021. "Antidepressant actions of ketamine engage cell-specific translation via eIF4E," Nature, Nature, vol. 590(7845), pages 315-319, February.
    • Handle: RePEc:nat:nature:v:590:y:2021:i:7845:d:10.1038_s41586-020-03047-0
    DOI: 10.1038/s41586-020-03047-0
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