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心脏细胞亚细胞钙循环的随机耦合映射模型。

Stochastic coupled map model of subcellular calcium cycling in cardiac cells.

作者信息

Romero Luis, Alvarez-Lacalle Enric, Shiferaw Yohannes

机构信息

Department of Physics, California State University, Northridge, California 91330, USA.

Departament de Fisica, Universitat Politècnica de Catalunya, BarcelonaTech, 08028 Barcelona, Spain.

出版信息

Chaos. 2019 Feb;29(2):023125. doi: 10.1063/1.5063462.

Abstract

In this study, we analyze a nonlinear map model of intracellular calcium (Ca) and voltage in cardiac cells. In this model, Ca release from the sarcoplasmic reticulum (SR) occurs at spatially distributed dyadic junctions that are diffusively coupled. At these junctions, release occurs with a probability that depends on key variables such as the SR load and the diastolic interval. Using this model, we explore how nonlinearity and stochasticity determine the spatial distribution of Ca release events within a cardiac cell. In particular, we identify a novel synchronization transition, which occurs at rapid pacing rates, in which the global Ca transient transitions from a period 2 response to a period 1 response. In the global period 2 response dyadic junctions fire in unison, on average, on alternate beats, while in the period 1 regime, Ca release at individual dyads is highly irregular. A close examination of the spatial distribution of Ca reveals that in the period 1 regime, the system coarsens into spatially out-of-phase regions with a length scale much smaller than the system size, but larger than the spacing between dyads. We have also explored in detail the coupling to membrane voltage. We study first the case of positive coupling, where a large Ca transient promotes a long action potential duration (APD). Here, the coupling to voltage synchronizes Ca release so that the system exhibits a robust period 2 response that is independent of initial conditions. On the other hand, in the case of negative coupling, where a large Ca transient tends to shorten the APD, we find a multitude of metastable states which consist of complex spatially discordant alternans patterns. Using an analogy to equilibrium statistical mechanics, we show that the spatial patterns observed can be explained by a mapping to the Potts model, with an additional term that accounts for a global coupling of spin states. Using this analogy, we argue that Ca cycling in cardiac cells exhibits complex spatiotemporal patterns that emerge via first or second order phase transitions. These results show that voltage and Ca can interact in order to induce complex subcellular responses, which can potentially lead to heart rhythm disorders.

摘要

在本研究中,我们分析了心脏细胞内钙离子(Ca)和电压的非线性映射模型。在该模型中,肌浆网(SR)的Ca释放发生在通过扩散耦合的空间分布二元连接处。在这些连接处,释放以取决于诸如SR负荷和舒张间期等关键变量的概率发生。利用该模型,我们探究了非线性和随机性如何决定心脏细胞内Ca释放事件的空间分布。特别地,我们识别出一种新的同步转变,其发生在快速起搏速率下,其中全局Ca瞬变从周期2响应转变为周期1响应。在全局周期2响应中,二元连接处平均每隔一拍同步放电,而在周期1状态下,单个二元处的Ca释放高度不规则。对Ca空间分布的仔细检查表明,在周期1状态下,系统粗化为空间异相区域,其长度尺度远小于系统大小,但大于二元之间的间距。我们还详细探究了与膜电压的耦合。我们首先研究正耦合的情况,即大的Ca瞬变促进长动作电位时程(APD)。在此,与电压的耦合使Ca释放同步,从而系统呈现出与初始条件无关的稳健周期2响应。另一方面,在负耦合的情况下,即大的Ca瞬变倾向于缩短APD,我们发现了许多亚稳态,它们由复杂的空间不协调交替模式组成。通过类比平衡统计力学,我们表明观察到的空间模式可以通过映射到Potts模型来解释,其中有一个额外的项来解释自旋态的全局耦合。利用这种类比,我们认为心脏细胞中的Ca循环呈现出通过一阶或二阶相变出现的复杂时空模式。这些结果表明电压和Ca可以相互作用以诱导复杂的亚细胞反应,这可能潜在地导致心律失常。

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Nonlinear onset of calcium wave propagation in cardiac cells.钙离子波在心脏细胞中的非线性传播起始。
Phys Rev E. 2016 Sep;94(3-1):032405. doi: 10.1103/PhysRevE.94.032405. Epub 2016 Sep 14.
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Criticality in intracellular calcium signaling in cardiac myocytes.心肌细胞细胞内钙离子信号的关键作用。
Biophys J. 2012 Jun 6;102(11):2433-42. doi: 10.1016/j.bpj.2012.05.001. Epub 2012 Jun 5.
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Alternans and arrhythmias: from cell to heart.交替和心律失常:从细胞到心脏。
Circ Res. 2011 Jan 7;108(1):98-112. doi: 10.1161/CIRCRESAHA.110.223586.

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