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Model-based prediction of maximum pool size in the ribbon synapse

The synaptic ribbon is a specialized structure in photoreceptor neurons that tethers vesicles prior to release (Figure 1A). When a cell is stimulated, vesicles are released from the ribbon and later replenished from the population of mobile vesicles in the synaptic terminal. A train of depolarizing pulses causes the ribbon to alternate between periods of release (lasting Δt = 25 ms) and replenishment (lasting T = 50ms), which occur on estimated timescales of τr = 5 ms (for release) and τa = 815 ms (for replenishment). After the first few pulses, the system approaches a limit cycle, and the amount of vesicles released on each pulse converges to a limiting value, R (Figure 1B). This can be used to determine the maximum available pool size on the ribbon, A. The standard method for estimating A is to measure the rate of replenishment in the limit, and then back-extrapolate from the cumulative release plot to obtain the available pool size at the start of the pulse train [1]. When comparing pulse trains of different strengths, this method yields substantially different values for A, a somewhat paradoxical result. Back-extrapolation assumes, however, that the replenishment rate is constant, even though it is thought to be proportional to the available space on the ribbon [2].

Table 1 Maximum pool size predictions from pulse train data
Figure 1
figure 1

A) The synaptic ribbon. (B) The available pool size, A(t), during a stimulus pulse train.

We developed a model-based approach to estimate A from the limiting release R. We modeled the rate of release (resp. replenishment) to simply be proportional to the number of vesicles on the ribbon (resp. vacant ribbon sites), and using the measured timescale τr (resp. τa). By solving the alternating differential equations, we derived a recurrence relation for the release during each pulse, Ri, which we then solved to obtain a closed form expression for Ri and the limiting release R. Specifically, we found that A = cR, where c is a function of τr,τa,Δt,T, and p, with p a release constant that captures the stimulus dependence of release probabilities, and can be estimated from the first release, R1. In contrast to the back-extrapolation method, our model-based estimate for A was similar across stimulus types (Table 1), while p was much smaller for the weaker stimulus. This suggests that available pool size does not change with stimulus strength; instead, differences in release result from changes in release probability.

References

  1. Sakaba T, Schneggenburger R, Neher E: Estimation of quantal parameters at the calyx of Held synapse. Neurosci Res. 2002, 44 (4): 343-356.

    Article  PubMed  Google Scholar 

  2. Van Hook MJ, Parmelee CM, Chen M, Cork KM, Curto C, Thoreson WB: Calmodulin enhances ribbon replenishment and shapes filtering of synaptic transmission by cone photoreceptors. J Gen Physiol. 2014, 144 (5): 357-378.

    Article  PubMed  CAS  PubMed Central  Google Scholar 

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Correspondence to Caitlyn M Parmelee.

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Parmelee, C.M., Van Hook, M., Thoreson, W.B. et al. Model-based prediction of maximum pool size in the ribbon synapse. BMC Neurosci 16 (Suppl 1), P41 (2015). https://0-doi-org.brum.beds.ac.uk/10.1186/1471-2202-16-S1-P41

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