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Ca2+ Dynamics in a Population of Smooth Muscle Cells: Modeling the Recruitment and Synchronization

机译:平滑肌细胞群体中的Ca2 +动力学:招聘和同步建模。

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摘要

Many experimental studies have shown that arterial smooth muscle cells respond with cytosolic calcium rises to vasoconstrictor stimulation. A low vasoconstrictor concentration gives rise to asynchronous spikes in the calcium concentration in a few cells (asynchronous flashing). With a greater vasoconstrictor concentration, the number of smooth muscle cells responding in this way increases (recruitment) and calcium oscillations may appear. These oscillations may eventually synchronize and generate arterial contraction and vasomotion. We show that these phenomena of recruitment and synchronization naturally emerge from a model of a population of smooth muscle cells coupled through their gap junctions. The effects of electrical, calcium, and inositol 1,4,5-trisphosphate coupling are studied. A weak calcium coupling is crucial to obtain a synchronization of calcium oscillations and the minimal required calcium permeability is deduced. Moreover, we note that an electrical coupling can generate oscillations, but also has a desynchronizing effect. Inositol 1,4,5-trisphosphate diffusion does not play an important role to achieve synchronization. Our model is validated by published in vitro experiments obtained on rat mesenteric arterial segments.
机译:许多实验研究表明,动脉平滑肌细胞对溶质钙的刺激会引起血管收缩刺激。血管收缩剂浓度低会导致少数细胞中钙浓度的异步峰值(异步闪烁)。随着血管收缩剂浓度的增加,以这种方式反应的平滑肌细胞数量增加(招募),并且可能出现钙振荡。这些振荡最终可能会同步并产生动脉收缩和血管舒缩。我们表明,这些募集和同步现象自然是从通过其缝隙连接处耦合的平滑肌细胞群体的模型中自然产生的。研究了电,钙和肌醇1,4,5-三磷酸酯偶联的影响。弱的钙偶合对于获得钙振荡的同步性至关重要,并且推导出所需的最小钙渗透率。此外,我们注意到电耦合会产生振荡,但也会产生失步效应。肌醇1,4,5-三磷酸酯的扩散对于实现同步化没有重要作用。我们的模型通过在大鼠肠系膜动脉节段上获得的已发表的体外实验进行了验证。

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