Nature Communications (Jun 2023)

Tetraspanin-8 sequesters syntaxin-2 to control biphasic release propensity of mucin granules

  • José Wojnacki,
  • Agustin Leonardo Lujan,
  • Nathalie Brouwers,
  • Carla Aranda-Vallejo,
  • Gonzalo Bigliani,
  • Maria Pena Rodriguez,
  • Ombretta Foresti,
  • Vivek Malhotra

DOI
https://doi.org/10.1038/s41467-023-39277-9
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 17

Abstract

Read online

Abstract Agonist-mediated stimulated pathway of mucin and insulin release are biphasic in which rapid fusion of pre-docked granules is followed by slow docking and fusion of granules from the reserve pool. Here, based on a cell-culture system, we show that plasma membrane-located tetraspanin-8 sequesters syntaxin-2 to control mucin release. Tetraspanin-8 affects fusion of granules during the second phase of stimulated mucin release. The tetraspanin-8/syntaxin-2 complex does not contain VAMP-8, which functions with syntaxin-2 to mediate granule fusion. We suggest that by sequestering syntaxin-2, tetraspanin-8 prevents docking of granules from the reserve pool. In the absence of tetraspanin-8, more syntaxin-2 is available for docking and fusion of granules and thus doubles the quantities of mucins secreted. This principle also applies to insulin release and we suggest a cell type specific Tetraspanin/Syntaxin combination is a general mechanism regulating the fusion of dense core granules.