PLoS Biology (Apr 2023)

The active zone protein Clarinet regulates synaptic sorting of ATG-9 and presynaptic autophagy

  • Zhao Xuan,
  • Sisi Yang,
  • Benjamin Clark,
  • Sarah E. Hill,
  • Laura Manning,
  • Daniel A. Colón-Ramos

Journal volume & issue
Vol. 21, no. 4

Abstract

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Autophagy is essential for cellular homeostasis and function. In neurons, autophagosome biogenesis is temporally and spatially regulated to occur near presynaptic sites, in part via the trafficking of autophagy transmembrane protein ATG-9. The molecules that regulate autophagy by sorting ATG-9 at synapses remain largely unknown. Here, we conduct forward genetic screens at single synapses of C. elegans neurons and identify a role for the long isoform of the active zone protein Clarinet (CLA-1L) in regulating sorting of autophagy protein ATG-9 at synapses, and presynaptic autophagy. We determine that disrupting CLA-1L results in abnormal accumulation of ATG-9 containing vesicles enriched with clathrin. The ATG-9 phenotype in cla-1(L) mutants is not observed for other synaptic vesicle proteins, suggesting distinct mechanisms that regulate sorting of ATG-9-containing vesicles and synaptic vesicles. Through genetic analyses, we uncover the adaptor protein complexes that genetically interact with CLA-1 in ATG-9 sorting. We also determine that CLA-1L extends from the active zone to the periactive zone and genetically interacts with periactive zone proteins in ATG-9 sorting. Our findings reveal novel roles for active zone proteins in the sorting of ATG-9 and in presynaptic autophagy. Autophagosome biogenesis is temporally and spatially regulated to occur near presynaptic sites in neurons. This study identifies novel roles for active zone proteins in specifically regulating activity-dependent presynaptic autophagy via sorting of the autophagy protein ATG-9.