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从离子到人类心房心肌细胞的细胞变异性:综合计算和实验研究。

From ionic to cellular variability in human atrial myocytes: an integrative computational and experimental study.

机构信息

Department of Computer Science, University of Oxford , Oxford , United Kingdom.

Division of Cardiovascular Medicine, Radcliffe Department of Medicine, University of Oxford, John Radcliffe Hospital , Oxford , United Kingdom.

出版信息

Am J Physiol Heart Circ Physiol. 2018 May 1;314(5):H895-H916. doi: 10.1152/ajpheart.00477.2017. Epub 2017 Dec 22.

Abstract

Variability refers to differences in physiological function between individuals, which may translate into different disease susceptibility and treatment efficacy. Experiments in human cardiomyocytes face wide variability and restricted tissue access; under these conditions, computational models are a useful complementary tool. We conducted a computational and experimental investigation in cardiomyocytes isolated from samples of the right atrial appendage of patients undergoing cardiac surgery to evaluate the impact of variability in action potentials (APs) and subcellular ionic densities on Ca transient dynamics. Results showed that 1) variability in APs and ionic densities is large, even within an apparently homogenous patient cohort, and translates into ±100% variation in ionic conductances; 2) experimentally calibrated populations of models with wide variations in ionic densities yield APs overlapping with those obtained experimentally, even if AP characteristics of the original generic model differed significantly from experimental APs; 3) model calibration with AP recordings restricts the variability in ionic densities affecting upstroke and resting potential, but redundancy in repolarization currents admits substantial variability in ionic densities; and 4) model populations constrained with experimental APs and ionic densities exhibit three Ca transient phenotypes, differing in intracellular Ca handling and Na/Ca membrane extrusion. These findings advance our understanding of the impact of variability in human atrial electrophysiology. NEW & NOTEWORTHY Variability in human atrial electrophysiology is investigated by integrating for the first time cellular-level and ion channel recordings in computational electrophysiological models. Ion channel calibration restricts current densities but not cellular phenotypic variability. Reduced Na/Ca exchanger is identified as a primary mechanism underlying diastolic Ca fluctuations in human atrial myocytes.

摘要

变异性是指个体之间生理功能的差异,这可能转化为不同的疾病易感性和治疗效果。在人类心肌细胞中进行实验面临着广泛的变异性和有限的组织获取;在这些条件下,计算模型是一种有用的补充工具。我们在接受心脏手术的患者右心耳样本中分离的心肌细胞中进行了计算和实验研究,以评估动作电位(APs)和亚细胞离子密度变异性对 Ca 瞬变动力学的影响。结果表明:1)即使在明显同质的患者群体中,APs 和离子密度的变异性也很大,转化为离子电导的±100%变化;2)用具有广泛离子密度变化的实验校准的模型群体产生与实验获得的重叠的 APs,即使原始通用模型的 AP 特征与实验 APs 有很大差异;3)用 AP 记录进行模型校准限制了影响上升和静息电位的离子密度的变异性,但复极化电流的冗余允许离子密度有很大的变异性;4)用实验 APs 和离子密度约束的模型群体表现出三种 Ca 瞬变表型,在细胞内 Ca 处理和 Na/Ca 膜外排方面存在差异。这些发现提高了我们对人类心房电生理学变异性影响的理解。

新的和值得注意的是

通过首次在计算电生理学模型中整合细胞水平和离子通道记录来研究人类心房电生理学的变异性。离子通道校准限制了电流密度,但不限制细胞表型变异性。减少的 Na/Ca 交换体被确定为人类心房心肌细胞舒张期 Ca 波动的主要机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/095b/6008144/532c98f8a08d/zh40031824430001.jpg

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