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Autophagy within the mushroom body protects from synapse aging in a non-cell autonomous manner

Author

Listed:
  • Anuradha Bhukel

    (Freie Universität Berlin
    NeuroCure, Charité)

  • Christine Brigitte Beuschel

    (Freie Universität Berlin
    NeuroCure, Charité)

  • Marta Maglione

    (Freie Universität Berlin
    NeuroCure, Charité)

  • Martin Lehmann

    (Campus Berlin-Buch)

  • Gabor Juhász

    (Eötvös Loránd University)

  • Frank Madeo

    (University of Graz
    BioTechMed Graz)

  • Stephan J. Sigrist

    (Freie Universität Berlin
    NeuroCure, Charité)

Abstract

Macroautophagy is an evolutionarily conserved cellular maintenance program, meant to protect the brain from premature aging and neurodegeneration. How neuronal autophagy, usually loosing efficacy with age, intersects with neuronal processes mediating brain maintenance remains to be explored. Here, we show that impairing autophagy in the Drosophila learning center (mushroom body, MB) but not in other brain regions triggered changes normally restricted to aged brains: impaired associative olfactory memory as well as a brain-wide ultrastructural increase of presynaptic active zones (metaplasticity), a state non-compatible with memory formation. Mechanistically, decreasing autophagy within the MBs reduced expression of an NPY-family neuropeptide, and interfering with autocrine NPY signaling of the MBs provoked similar brain-wide metaplastic changes. Our results in an exemplary fashion show that autophagy-regulated signaling emanating from a higher brain integration center can execute high-level control over other brain regions to steer life-strategy decisions such as whether or not to form memories.

Suggested Citation

  • Anuradha Bhukel & Christine Brigitte Beuschel & Marta Maglione & Martin Lehmann & Gabor Juhász & Frank Madeo & Stephan J. Sigrist, 2019. "Autophagy within the mushroom body protects from synapse aging in a non-cell autonomous manner," Nature Communications, Nature, vol. 10(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-09262-2
    DOI: 10.1038/s41467-019-09262-2
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    Cited by:

    1. Áron Szabó & Virág Vincze & Aishwarya Sanjay Chhatre & András Jipa & Sarolta Bognár & Katalin Eszter Varga & Poulami Banik & Adél Harmatos-Ürmösi & Lukas J. Neukomm & Gábor Juhász, 2023. "LC3-associated phagocytosis promotes glial degradation of axon debris after injury in Drosophila models," Nature Communications, Nature, vol. 14(1), pages 1-19, December.

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