eLife (Aug 2021)

Reexamination of N-terminal domains of syntaxin-1 in vesicle fusion from central murine synapses

  • Gülçin Vardar,
  • Andrea Salazar-Lázaro,
  • Marisa Brockmann,
  • Marion Weber-Boyvat,
  • Sina Zobel,
  • Victor Wumbor-Apin Kumbol,
  • Thorsten Trimbuch,
  • Christian Rosenmund

DOI
https://doi.org/10.7554/eLife.69498
Journal volume & issue
Vol. 10

Abstract

Read online

Syntaxin-1 (STX1) and Munc18-1 are two requisite components of synaptic vesicular release machinery, so much so synaptic transmission cannot proceed in their absence. They form a tight complex through two major binding modes: through STX1’s N-peptide and through STX1’s closed conformation driven by its Habc- domain. However, physiological roles of these two reportedly different binding modes in synapses are still controversial. Here we characterized the roles of STX1’s N-peptide, Habc-domain, and open conformation with and without N-peptide deletion using our STX1-null mouse model system and exogenous reintroduction of STX1A mutants. We show, on the contrary to the general view, that the Habc-domain is absolutely required and N-peptide is dispensable for synaptic transmission. However, STX1A’s N-peptide plays a regulatory role, particularly in the Ca2+-sensitivity and the short-term plasticity of vesicular release, whereas STX1’s open conformation governs the vesicle fusogenicity. Strikingly, we also show neurotransmitter release still proceeds when the two interaction modes between STX1A and Munc18-1 are presumably intervened, necessitating a refinement of the conceptualization of STX1A–Munc18-1 interaction.

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