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Species-dependent adaptation of the cardiac Na+/K+ pump kinetics to the intracellular Na+ concentration

机译:心脏Na + / K +泵动力学对细胞内Na +浓度的物种依赖性适应

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The Na+/K+ ATPase (NKA) plays a critical role in maintaining ionic homeostasis and dynamic function in cardiac myocytes, within both the in vivo cell and in silico models. Physiological conditions differ significantly between mammalian species. However, most existing formulations of NKA used to simulate cardiac function in computational models are derived from a broad range of experimental sources spanning many animal species. The resultant inability of these models to discern species-specific features is a significant obstacle to achieving a detailed quantitative and comparative understanding of physiological behaviour in different biological contexts. Here we present a framework for characterising the steady-state NKA current using a biophysical mechanistic model specifically designed to provide a mechanistic explanation of the NKA flux supported by self-consistent species-specific data. We thus compared NKA kinetics specific to guinea- pig and rat ventricular myocytes. We observe that the apparent binding affinity for sodium in the rat is significantly lower, whereas the overall pump cycle rate is doubled, in comparison to the guinea pig. This sensitivity of NKA to its regulatory substrates compensates for the differences in Na+ concentrations between the cell types. NKA is thereby maintained within its dynamic range over a wide range of pacing frequencies in these two species, despite significant disparities in sodium concentration. Hence, by replacing a conventional generic NKA model with our rat-specific NKA formula into a whole-cell simulation, we have, for the first time, been able to accurately reproduce the action potential duration and the steady-state sodium concentration as functions of pacing frequency.
机译:在体内细胞模型和计算机模型中,Na + / K + ATPase(NKA)在维持心肌细胞的离子稳态和动态功能中都起着关键作用。哺乳动物之间的生理条件差异很大。但是,在计算模型中用于模拟心脏功能的NKA的大多数现有配方均来自横跨许多动物物种的广泛实验来源。这些模型导致的无法识别特定物种的特征,是在不同生物学环境下实现对生理行为的详细定量和比较理解的重大障碍。在这里,我们提出了一个使用生物物理力学模型表征稳态NKA电流的框架,该模型专门设计用于提供由自洽物种特异性数据支持的NKA通量的力学解释。因此,我们比较了豚鼠和大鼠心室肌细胞特有的NKA动力学。我们观察到,与豚鼠相比,大鼠对钠的表观结合亲和力明显更低,而总泵循环速率却翻了一番。 NKA对调节底物的这种敏感性补偿了细胞类型之间Na +浓度的差异。因此,尽管钠浓度存在显着差异,但在这两个物种的大范围起搏频率范围内,NKA仍保持在其动态范围内。因此,通过用大鼠特有的NKA公式代替传统的普通NKA模型进入全细胞模拟,我们首次能够准确地再现动作电位持续时间和稳态钠浓度作为起搏频率。

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