SNAP-25 is expressed in islets of Langerhans and is involved in insulin release.

K Sadoul, J Lang, C Montecucco, U Weller… - The Journal of cell …, 1995 - rupress.org
K Sadoul, J Lang, C Montecucco, U Weller, R Regazzi, S Catsicas, CB Wollheim, PA Halban
The Journal of cell biology, 1995rupress.org
SNAP-25 is known as a neuron specific molecule involved in the fusion of small synaptic
vesicles with the presynaptic plasma membrane. By immunolocalization and Western blot
analysis, it is now shown that SNAP-25 is also expressed in pancreatic endocrine cells.
Botulinum neurotoxins (BoNT) A and E were used to study the role of SNAP-25 in insulin
secretion. These neurotoxins inhibit transmitter release by cleaving SNAP-25 in neurons.
Cells from a pancreatic B cell line (HIT) and primary rat islet cells were permeabilized with …
SNAP-25 is known as a neuron specific molecule involved in the fusion of small synaptic vesicles with the presynaptic plasma membrane. By immunolocalization and Western blot analysis, it is now shown that SNAP-25 is also expressed in pancreatic endocrine cells. Botulinum neurotoxins (BoNT) A and E were used to study the role of SNAP-25 in insulin secretion. These neurotoxins inhibit transmitter release by cleaving SNAP-25 in neurons. Cells from a pancreatic B cell line (HIT) and primary rat islet cells were permeabilized with streptolysin-O to allow toxin entry. SNAP-25 was cleaved by BoNT/A and BoNT/E, resulting in a molecular mass shift of approximately 1 and 3 kD, respectively. Cleavage was accompanied by an inhibition of Ca(++)-stimulated insulin release in both cell types. In HIT cells, a concentration of 30-40 nM BoNT/E gave maximal inhibition of stimulated insulin secretion of approximately 60%, coinciding with essentially complete cleavage of SNAP-25. Half maximal effects in terms of cleavage and inhibition of insulin release were obtained at a concentration of 5-10 nM. The A type toxin showed maximal and half-maximal effects at concentrations of 4 and 2 nM, respectively. In conclusion, the results suggest a role for SNAP-25 in fusion of dense core secretory granules with the plasma membrane in an endocrine cell type- the pancreatic B cell.
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