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Diabetes, Vol 49, Issue 9 1500-1510, Copyright © 2000 by American Diabetes Association
Tight coupling between electrical activity and exocytosis in mouse glucagon-secreting alpha-cells
S Barg, J Galvanovskis, SO Gopel, P Rorsman and L Eliasson
Department of Molecular and Cellular Physiology, Institute of Physiological Sciences, University of Lund, Sweden.
alpha-Cells were identified in preparations of dispersed mouse islets by
immunofluorescence microscopy. A high fraction of alpha-cells correlated
with a small cell size measured as the average cell diameter (10 microm)
and whole-cell capacitance (<4 pF). The alpha-cells generated action
potentials at a low frequency (1 Hz) in the absence of glucose. These
action potentials were reversibly inhibited by elevation of the glucose
concentration to 20 mmol/l. The action potentials originated from a
membrane potential more negative than -50 mV, had a maximal upstroke
velocity of 5 V/s, and peaked at +1 mV. Voltage-clamp experiments revealed
the ionic conductances underlying the generation of action potentials.
alpha-Cells are equipped with a delayed tetraethyl-ammonium-blockable
outward current (activating at voltages above -20 mV), a large
tetrodotoxin-sensitive Na+ current (above -30 mV; peak current 200 pA at
+10 mV), and a small Ca2+ current (above -50 mV; peak current 30 pA at +10
mV). The latter flowed through omega-conotoxin GVIA (25%)- and
nifedipine-sensitive (50%) Ca(2+)-channels. Mouse alpha-cells contained, on
average, 7,300 granules, which undergo Ca(2+)-induced exocytosis when the
alpha-cell is depolarized. Three functional subsets of granules were
identified, and the size of the immediately releasable pool was estimated
as 80 granules, or 1% of the total granule number. The maximal rate of
exocytosis (1.5 pF/s) was observed 21 ms after the onset of the
voltage-clamp depolarization, which is precisely the duration of
Ca(2+)-influx during an action potential. Our results suggest that the
secretory machinery of the alpha-cell is optimized for maximal efficiency
in the use of Ca2+ for exocytosis.

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Copyright © 2000 by the American Diabetes Association.
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