AI Article Synopsis

  • The study examined mouse diaphragm muscles to understand how motor nerve endings manage neurotransmitter release and vesicle recycling during continuous stimulation at a rate of 20 impulses per second.
  • There were three distinct phases observed in endplate potential (EPP) amplitudes: a quick drop during initial stimulation, a stable plateau for 1-2 minutes, and a gradual decline afterward.
  • The findings indicated that mouse motor nerve endings have a high rate of synaptic vesicle endocytosis and recycling (around 50 seconds on average), essential for maintaining effective neurotransmission during prolonged, high-frequency activity.

Article Abstract

Experiments on the mouse diaphragm muscle using intracellular microelectrode recordings and fluorescence microscopy were performed to study the dynamics of transmitter secretion and synaptic vesicle recycling processes (the exocytosis-endocytosis cycle) in motor nerve endings (NE) during prolonged rhythmic stimulation (20 impulses/sec). During stimulation, there were triphasic changes in the amplitude of endplate potentials (EPP): an initial rapid reduction, followed by prolonged (1-2 min) stabilization of amplitude, i.e., a plateau, and then a further slow decrease. Restoration of EPP amplitude after stimulation for 3 min occurred over a period of several seconds. Loading of synaptic vesicles with the fluorescent endocytic stain FM1-43 showed that rhythmic stimulation led to a gradual (over 5-6 min) decrease in NE fluorescence, demonstrating exocytosis of synaptic vesicles. Quantum analysis of the electrophysiological data and comparison of these data with results from fluorescence studies suggested that mouse NE have a high rate of endocytosis and reutilization of synaptic vesicles (the mean recycling time was about 50 sec), which may support the maintenance of reliable synaptic transmission during prolonged high-frequency activity. The sizes of the release-ready and recycling pools of synaptic vesicles were determined quantitatively. It is suggested that vesicle recycling in mouse NE occurs via a short, rapid pathway with incorporation into the recycling pool. Vesicles of the reserve pool are not used for transmitter secretion in the stimulation conditions used here.

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Source
http://dx.doi.org/10.1007/s11055-009-9122-xDOI Listing

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