Synaptic activity slows vesicular replenishment at excitatory synapses of rat hippocampus
Short-term synaptic depression mainly reflects the depletion of the readily releasable pool (RRP) of quanta. Its dynamics, and especially the replenishment rate of the RRP, are still not well characterized in spite of decades of investigation. Main reason is that the vesicular storage and release system is treated as time-independent. If it is time-dependent all parameters thus estimated become problematic. Indeed the reports about how prolonged stimulation affects the dynamics are contradictory. To study this, we used patterned stimulation on the Schaeffer collateral fiber pathway and model-fitting of the excitatory post-synaptic currents (EPSC) recorded from CA1 neurons in rat hippocampal slices. The parameters of a vesicular storage and release model with two pools were estimated by minimizing the squared difference between the ESPC amplitudes and simulated model output. This yields the 'basic' parameters (release coupling, replenishment coupling and RRP size) that underlie the 'derived' and commonly used parameters (fractional release and replenishment rate). The fractional release increases when [Ca ?? ] o is raised, whereas the replenishment rate is [Ca ?? ] o independent. Fractional release rises because release coupling increases, and the RRP becomes less able to contain quanta. During prolonged stimulation, the fractional release remains generally unaltered, whereas the replenishment rate decreases down to *10 % of its initial value with a decay time of *15 s, and this decrease in the replenishment rate significantly contributes to synaptic depression. In conclusion, the fractional release is [Ca ?? ] odependent and stimulation-independent, whereas the replenishment rate is [Ca ?? ] o -independent and stimulation-dependent.
At the excitatory synapse of rat hippocampus the short-term synaptic depression observed during long high-frequency stimulation is associated with slower replenishment of the readily-releasable pool. Given that the replenishment rate is also not [Ca(++)]o sensitive this puts into question a widely held notion that the vesicles-constrained by the cytoskeleton and rendered free from such constraints by Ca(++) entry that renders them more mobile-are important in the replenishment of the readily-releasable pool. This raises a question-Is vesicular replenishment of the readily releasable pool associated with significant movement? To answer this question we evaluated how okadaic acid and staurosporine (compounds known to affect vesicular mobility) influence the replenishment rate. We used patterned stimulation on the Schaffer collateral fiber pathway and recorded the excitatory post-synaptic currents (EPSCs) from rat CA1 neurons, in the absence and presence of these drugs. The parameters of a circuit model with two vesicular pools were estimated by minimizing the squared difference between the ESPC amplitudes and simulated model output. [Ca(2+)]o did not influence the progressive decrease of the replenishment rate during long, high frequency stimulation. Okadaic acid did not significantly affect any parameters of the vesicular storage and release system, including the replenishment rate. Staurosporine reduced the replenishment coupling, but not the replenishment rate, and this is owing to the fact that it also reduces the ability of the readily releasable pool to contain quanta. Moreover, these compounds were ineffective in influencing how the replenishment rate decreases during long, high frequency stimulation. In conclusion at the excitatory synapses of rat hippocampus the replenishment of the readily releasable pool does not appear to be associated with a significant vesicular movement, and during long high frequency stimulation [Ca(++)]o does not influence the progressive decrease of vesicular replenishment.
How vesicular dynamics parameters depend on temperature and how temperature affects the parameter change during prolonged high frequency stimulation was determined by fitting a model of vesicular storage and release to the amplitudes of the excitatory post-synaptic currents (EPSC) recorded from CA1 neurons in rat hippocampal slices. The temperature ranged from low (13 °C) to higher and more physiological temperature (34 °C). Fitting the model of vesicular storage and release to the EPSC amplitudes during a single pair of brief high-low frequency stimulation trains yields the estimates of all parameters of the vesicular dynamics, and with good precision. Both fractional release and replenishment rate decrease as the temperature rises. Change of the underlying 'basic' parameters (release coupling, replenishment coupling and readily releasable pool size), which the model-fitting also yields is complex. The replenishment coupling between the readily releasable pool (RRP) and resting pool increases with temperature (which renders the replenishment rate higher), but this is more than counterbalanced by greater RRP size (which renders the replenishment rate lower). Finally, during long, high frequency patterned stimulation that leads to significant synaptic depression, the replenishment rate decreases markedly and rapidly at low temperatures (<22 °C), but at high temperatures (>28 °C) the replenishment rate rises with stimulation, making synapses better able to maintain synaptic efficacy.
Recovery of vesicular storage and release parameters after high frequency stimulation in rat hippocampus
The replenishment rates estimated from the recovery of synaptic efficacy following synaptic depression are known to be widely scattered. Given the importance of the replenishment during stimulation, especially if it is prolonged, it is important to better understand what influences the recovery of the synaptic efficacy following stimulation. We fit a two-pool model of vesicular secretion to the changes of the excitatory post-synaptic currents recorded in CA1 neurons of rat hippocampal slices to determine how the model parameters change during, and following, long stimulation. The replenishment rate at the end of stimulation inducing synaptic depression differs greatly from that at the beginning of stimulation. It decreases progressively and rapidly (by ~75 % and with a time constant of <10 s) during stimulation, and this is followed by a similarly fast recovery (time constant of ~10 s), but to a steady-state that is approximately twice as large as its pre-stimulation value. Both [Ca(++)]o and the duration of long stimulation influence the recovery of the replenishment rate. Its new steady-state is significantly higher, if either [Ca(++)]o is higher or stimulation longer, but the recovery of the replenishment rate becomes clearly slower if [Ca(++)]o is higher, and faster if stimulation is longer. Many factors thus influence the recovery of the replenishment rate and of the synaptic efficacy, but the stimulation induced [Ca(++)]i accumulation cannot explain the change of the replenishment rate during recovery. Finally, okadaic acid, which speeds up vesicular trafficking, does not alter the recovery of the replenishment rate. The vesicular replenishment of the RRP following stimulation is thus not likely to be associated with significant vesicular movement.
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