DeRemigio Hilary, Smith Gregory D
Department of Applied Science, McGlothlin-Street Hall, The College of William and Mary, Williamsburg, VA 23187, USA.
Cell Calcium. 2005 Aug;38(2):73-86. doi: 10.1016/j.ceca.2005.06.007.
Localized Ca(2+) elevations known as Ca(2+) puffs and sparks are cellular signals that arise from the cooperative activity of clusters of inositol 1,4,5-trisphosphate receptors and ryanodine receptors clustered at Ca(2+) release sites on the surface of the endoplasmic reticulum or sarcoplasmic reticulum. When Markov chain models of these intracellular Ca(2+)-regulated Ca(2+) channels are coupled via a mathematical representation of Ca(2+) microdomain, simulated Ca(2+) release sites may exhibit the phenomenon of "stochastic Ca(2+) excitability" where the inositol 1,4,5-trisphosphate receptors (IP(3)Rs) or ryanodine receptors (RyRs) open and close in a concerted fashion. Interestingly, under some conditions simulated puffs and sparks can be observed even when the single-channel model used does not include slow Ca(2+) inactivation or, indeed, any long-lived closed/refractory state [V. Nguyen, R. Mathias, G. Smith, Stochastic automata network descriptor for Markov chain models of instantaneously-coupled intracellular Ca(2+) channels, Bull. Math. Biol. 67 (2005) 393-432]. In this case, termination of the localized Ca(2+) elevation occurs when all of the intracellular channels at a release site simultaneously close through a process referred to as stochastic attrition [M. Stern, Theory of excitation-contraction coupling in cardiac muscle, Biophys. J. 63 (1992) 497-517]. In this paper, we investigate the statistical properties of stochastic attrition viewed as an absorption time on a terminating Markov chain that represents a Ca(2+) release site composed of N two-state channels that are activated by Ca(2+). Assuming that the local [Ca(2+)] experienced by a channel depends only on the number of open channels at the Ca(2+) release site (i.e., instantaneous mean-field coupling [ibid.], we derive the probability distribution function for the time until stochastic attrition occurs and present an analytical formula for the expectation of this random variable. We explore how the contribution of stochastic attrition to the termination of Ca(2+) puffs and sparks depends on the number of channels at a release site, the source amplitude of the channels (i.e., the strength of the coupling), the background [Ca(2+)], channel kinetics, and the cooperactivity of Ca(2+) binding. Because we explicitly model the Ca(2+) regulation of the intracellular channels, our results differ markedly from (and in fact generalize) preliminary analyses that assume the intracellular Ca(2+) channels are uncoupled and consequently independent.
局部钙离子浓度升高,即所谓的“钙离子脉冲”和“钙离子闪烁”,是细胞信号,它们源于聚集在内质网或肌浆网表面钙离子释放位点上的肌醇1,4,5 -三磷酸受体和兰尼碱受体簇的协同活动。当这些细胞内钙离子调节的钙离子通道的马尔可夫链模型通过钙离子微区的数学表示进行耦合时,模拟的钙离子释放位点可能会表现出“随机钙离子兴奋性”现象,即肌醇1,4,5 -三磷酸受体(IP₃Rs)或兰尼碱受体(RyRs)以协同方式打开和关闭。有趣的是,在某些情况下,即使所使用的单通道模型不包括缓慢的钙离子失活,甚至不包括任何长寿命的关闭/不应期状态,也能观察到模拟的脉冲和闪烁现象[V. 阮、R. 马蒂亚斯、G. 史密斯,瞬时耦合细胞内钙离子通道马尔可夫链模型的随机自动机网络描述符,《数学生物学通报》67 (2005) 393 - 432]。在这种情况下,当释放位点处的所有细胞内通道通过一个称为随机磨损的过程同时关闭时,局部钙离子浓度升高就会终止[M. 斯特恩,心肌兴奋 - 收缩偶联理论,《生物物理杂志》63 (1992) 497 - 517]。在本文中,我们将随机磨损视为终止马尔可夫链上的吸收时间来研究其统计特性,该马尔可夫链表示由N个由钙离子激活的双态通道组成的钙离子释放位点。假设通道所经历的局部钙离子浓度仅取决于钙离子释放位点处开放通道的数量(即瞬时平均场耦合[同上]),我们推导出直到随机磨损发生的时间的概率分布函数,并给出该随机变量期望的解析公式。我们探讨随机磨损对钙离子脉冲和闪烁终止的贡献如何取决于释放位点处的通道数量、通道的源幅度(即耦合强度)、背景钙离子浓度、通道动力学以及钙离子结合的协同性。因为我们明确地对细胞内通道的钙离子调节进行了建模,所以我们的结果与那些假设细胞内钙离子通道未耦合因而相互独立的初步分析有显著不同(实际上是对其进行了推广)。
