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具有真实横管的心室肌细胞钙离子动力学的多尺度建模。

Multiscale modeling of calcium dynamics in ventricular myocytes with realistic transverse tubules.

机构信息

Department of Computer Science, University of Wisconsin-Milwaukee, Milwaukee, WI 53211, USA.

出版信息

IEEE Trans Biomed Eng. 2011 Oct;58(10):2947-51. doi: 10.1109/TBME.2011.2158316. Epub 2011 May 31.

Abstract

Spatial-temporal Ca(2+) dynamics due to Ca(2+) release, buffering, and reuptaking plays a central role in studying excitation-contraction (E-C) coupling in both normal and diseased cardiac myocytes. In this paper, we employ two numerical methods, namely, the meshless method and the finite element method, to model such Ca(2+) behaviors by solving a nonlinear system of reaction-diffusion partial differential equations at two scales. In particular, a subcellular model containing several realistic transverse tubules (or t-tubules) is investigated and assumed to reside at different locations relative to the cell membrane. To this end, the Ca(2+) concentration calculated from the whole-cell modeling is adopted as part of the boundary constraint in the subcellular model. The preliminary simulations show that Ca(2+) concentration changes in ventricular myocytes are mainly influenced by calcium release from t-tubules.

摘要

由于钙释放、缓冲和再摄取引起的时空 Ca(2+)动力学在研究正常和患病心肌细胞中的兴奋-收缩(E-C)偶联中起着核心作用。在本文中,我们采用了两种数值方法,即无网格方法和有限元方法,通过求解两个尺度上的非线性反应扩散偏微分方程组来模拟这种 Ca(2+)行为。特别是,研究了一个包含几个现实的横管(或 t-管)的亚细胞模型,并假设其相对于细胞膜位于不同的位置。为此,采用从全细胞建模中计算出的 Ca(2+)浓度作为亚细胞模型中边界约束的一部分。初步的模拟表明,心室肌细胞中 Ca(2+)浓度的变化主要受 t-管中钙释放的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3262/3179564/41511f69bf29/nihms308491f1.jpg

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本文引用的文献

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Multiscale modeling in rodent ventricular myocytes.啮齿类动物心室肌细胞中的多尺度建模
IEEE Eng Med Biol Mag. 2009 Mar-Apr;28(2):46-57. doi: 10.1109/MEMB.2009.931787.
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Calcium cycling and signaling in cardiac myocytes.心肌细胞中的钙循环与信号传导。
Annu Rev Physiol. 2008;70:23-49. doi: 10.1146/annurev.physiol.70.113006.100455.
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Interplay of ryanodine receptor distribution and calcium dynamics.兰尼碱受体分布与钙动力学的相互作用。
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