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Determinants of synapse diversity revealed by super-resolution quantal transmission and active zone imaging

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  • Zachary L. Newman

    (University of California Berkeley)

  • Dariya Bakshinskaya

    (University of California Berkeley)

  • Ryan Schultz

    (University of California Berkeley)

  • Samuel J. Kenny

    (University of California)

  • Seonah Moon

    (University of California)

  • Krisha Aghi

    (University of California Berkeley)

  • Cherise Stanley

    (University of California Berkeley)

  • Nadia Marnani

    (University of California Berkeley)

  • Rachel Li

    (University of California Berkeley)

  • Julia Bleier

    (University of California Berkeley)

  • Ke Xu

    (University of California Berkeley
    University of California Berkeley
    University of California
    Lawrence Berkeley National Laboratory)

  • Ehud Y. Isacoff

    (University of California Berkeley
    University of California Berkeley
    Lawrence Berkeley National Laboratory
    University of California Berkeley)

Abstract

Neural circuit function depends on the pattern of synaptic connections between neurons and the strength of those connections. Synaptic strength is determined by both postsynaptic sensitivity to neurotransmitter and the presynaptic probability of action potential evoked transmitter release (Pr). Whereas morphology and neurotransmitter receptor number indicate postsynaptic sensitivity, presynaptic indicators and the mechanism that sets Pr remain to be defined. To address this, we developed QuaSOR, a super-resolution method for determining Pr from quantal synaptic transmission imaging at hundreds of glutamatergic synapses at a time. We mapped the Pr onto super-resolution 3D molecular reconstructions of the presynaptic active zones (AZs) of the same synapses at the Drosophila larval neuromuscular junction (NMJ). We find that Pr varies greatly between synapses made by a single axon, quantify the contribution of key AZ proteins to Pr diversity and find that one of these, Complexin, suppresses spontaneous and evoked transmission differentially, thereby generating a spatial and quantitative mismatch between release modes. Transmission is thus regulated by the balance and nanoscale distribution of release-enhancing and suppressing presynaptic proteins to generate high signal-to-noise evoked transmission.

Suggested Citation

  • Zachary L. Newman & Dariya Bakshinskaya & Ryan Schultz & Samuel J. Kenny & Seonah Moon & Krisha Aghi & Cherise Stanley & Nadia Marnani & Rachel Li & Julia Bleier & Ke Xu & Ehud Y. Isacoff, 2022. "Determinants of synapse diversity revealed by super-resolution quantal transmission and active zone imaging," Nature Communications, Nature, vol. 13(1), pages 1-18, December.
  • Handle: RePEc:nat:natcom:v:13:y:2022:i:1:d:10.1038_s41467-021-27815-2
    DOI: 10.1038/s41467-021-27815-2
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