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Stochastic Binding of Ca2+ Ions in the Dyadic Cleft; Continuous versus Random Walk Description of Diffusion

机译:二叉裂中Ca2 +离子的随机结合;扩散的连续与随机游动描述

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摘要

Ca2+ signaling in the dyadic cleft in ventricular myocytes is fundamentally discrete and stochastic. We study the stochastic binding of single Ca2+ ions to receptors in the cleft using two different models of diffusion: a stochastic and discrete Random Walk (RW) model, and a deterministic continuous model. We investigate whether the latter model, together with a stochastic receptor model, can reproduce binding events registered in fully stochastic RW simulations. By evaluating the continuous model goodness-of-fit for a large range of parameters, we present evidence that it can. Further, we show that the large fluctuations in binding rate observed at the level of single time-steps are integrated and smoothed at the larger timescale of binding events, which explains the continuous model goodness-of-fit. With these results we demonstrate that the stochasticity and discreteness of the Ca2+ signaling in the dyadic cleft, determined by single binding events, can be described using a deterministic model of Ca2+ diffusion together with a stochastic model of the binding events, for a specific range of physiological relevant parameters. Time-consuming RW simulations can thus be avoided. We also present a new analytical model of bimolecular binding probabilities, which we use in the RW simulations and the statistical analysis.
机译:Ca 2 + 信号在心室肌细胞的二叉形裂隙中基本上是离散且随机的。我们使用两种不同的扩散模型:随机离散离散漫游(RW)模型和确定性连续模型研究单个Ca 2 + 离子与裂隙中受体的随机结合。我们调查后一种模型,以及随机受体模型,是否可以重现完全随机RW模拟中记录的结合事件。通过评估大范围参数的连续模型拟合优度,我们提供了可以做到的证据。此外,我们表明,在单个时间步长水平上观察到的结合速率的大波动在更大的结合事件时间尺度上得到了整合和平滑,这说明了连续模型的拟合优度。这些结果表明,Ca 2 + 信号在二叉裂隙中的随机性和离散性(由单个结合事件确定)可以使用Ca 2+的确定性模型来描述。对于特定范围的生理相关参数,扩散与结合事件的随机模型一起。因此可以避免耗时的RW模拟。我们还提出了一种新的双分子结合概率分析模型,我们在RW模拟和统计分析中使用了该模型。

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