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The Journal of Neuroscience, October 15, 2001, 21(20):7889-7900
Estimation of Quantal Size and Number of Functional Active Zones
at the Calyx of Held Synapse by Nonstationary EPSC Variance
Analysis
Alexander C.
Meyer,
Erwin
Neher, and
Ralf
Schneggenburger
Max-Planck-Institut für biophysikalische Chemie, Abteilung
Membranbiophysik, D-37077 Göttingen, Germany
At the large excitatory calyx of Held synapse, the quantal size
during an evoked EPSC and the number of active zones contributing to
transmission are not known. We developed a nonstationary variant of
EPSC fluctuation analysis to determine these quantal parameters. AMPA
receptor-mediated EPSCs were recorded in slices of young (postnatal
8-10 d) rats after afferent fiber stimulation, delivered in trains to
induce synaptic depression. The means and the variances of EPSC
amplitudes were calculated across trains for each stimulus number.
During 10 Hz trains at 2 mM Ca2+
concentration ([Ca2+]), we found linear EPSC
variance-mean relationships, with a slope that was in good agreement
with the quantal size obtained from amplitude distributions of
spontaneous miniature EPSCs. At high release probability with 10 or 15 mM [Ca2+], competitive antagonists
were used to partially block EPSCs. Under these conditions, the EPSC
variance-mean plots could be fitted with parabolas, giving estimates
of quantal size and of the binomial parameter N. With
the rapidly dissociating antagonist kynurenic acid, quantal sizes were
larger than with a slowly dissociating antagonist, suggesting that the
effective glutamate concentration was increased at high release
probability. Considering the possibility of multivesicular release and
moderate saturation of postsynaptic AMPA receptors, we conclude
that the binomial parameter N (637 ± 117;
mean ± SEM) represents an upper limit estimate of the number of
functional active zones. We estimate that during normal synaptic transmission, the probability of vesicle fusion at single active zones
is in the range of 0.25-0.4.
Key words:
synaptic transmission; short-term depression; quantal
analysis; release probability; glutamate spillover; postsynaptic
currents; AMPA receptor
Copyright © 2001 Society for Neuroscience 0270-6474/01/21207889-12$05.00/0
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