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- Title
Small peptides patterned after the N-terminus domain of SNAP25 inhibit SNARE complex assembly and regulated exocytosis.
- Authors
Blanes-Mira, Clara; Merino, Jaime M.; Valera, Elvira; Fernandez-Ballester, Gregorio; Gutierrez, Luis M.; Viniegra, Salvador; Perez-Paya, Enrique; Ferrer-Montiel, Antonio
- Abstract
Synthetic peptides patterned after the C-terminus of synaptosomal associated protein of 25 kDa (SNAP25) efficiently abrogate regulated exocytosis. In contrast, the use of SNAP25 N-terminal-derived peptides to modulate SNAP receptors (SNARE) complex assembly and neurosecretion has not been explored. Here, we show that the N-terminus of SNAP25, specially the segment that encompasses 22Ala-44Ile, is essential for the formation of the SNARE complex. Peptides patterned after this protein domain are potent inhibitors of SNARE complex formation. The inhibitory activity correlated with their propensity to adopt an α-helical secondary structure. These peptides abrogated SNARE complex formation only when added previous to the onset of aggregate assembly. Analysis of the mechanism of action revealed that these peptides disrupted the binary complex formed by SNAP25 and syntaxin. The identified peptides inhibited Ca2+-dependent exocytosis from detergent-permeabilized excitable cells. Noteworthy, these amino acid sequences markedly protected intact hippocampal neurones against hypoglycaemia-induced, glutamate-mediated excitotoxicity with a potency that rivaled that displayed by botulinum neurotoxins. Our findings indicate that peptides patterned after the N-terminus of SNAP25 are potent inhibitors of SNARE complex formation and neuronal exocytosis. Because of their activity in intact neurones, these cell permeable peptides may be hits for antispasmodic and analgesic drug development.
- Subjects
SYNAPTOSOMES; PROTEINS; EXOCYTOSIS; PEPTIDES; PROTEIN-protein interactions
- Publication
Journal of Neurochemistry, 2004, Vol 88, Issue 1, p124
- ISSN
0022-3042
- Publication type
Article
- DOI
10.1046/j.1471-4159.2003.02133.x