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Role of single-channel stochastic noise on bursting clusters of pancreatic beta-cells.

机译:单通道随机噪声在胰腺β细胞的爆发簇中的作用。

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摘要

To study why pancreatic beta-cells prefer to burst as a multi-cellular complex, we have formulated a stochastic model for bursting clusters of excitable cells. Our model incorporated a delayed rectifier K+ channel, a fast voltage-gated Ca2+ channel, and a slow Cai-blockable Ca2+ channel. The fraction of ATP-sensitive K+ channels that may still be active in the bursting regime was included in the model as a leak current. We then developed an efficient method for simulating an ionic current component of an excitable cell that contains several thousands of channels opening simultaneously under unclamped voltage. Single channel open-close stochastic events were incorporated into the model by use of binomially distributed random numbers. Our simulations revealed that in an isolated beta-cell [Ca2+]i oscillates with a small amplitude about a low [Ca2+]i. However, in a large cluster of tightly coupled cells, stable bursts develop, and [Ca2+]i oscillates with a larger amplitude about a higher [Ca2+]i. This may explain why single beta-cells do not burst and also do not release insulin.
机译:为了研究为什么胰岛β细胞更喜欢以多细胞复合物的形式破裂,我们为破裂的可兴奋细胞簇建立了随机模型。我们的模型包含了一个延迟整流器K +通道,一个快速电压门控Ca2 +通道和一个缓慢的Cai可阻塞Ca2 +通道。 ATP敏感的K +通道在突发状态中可能仍处于活动状态的部分作为泄漏电流包含在模型中。然后,我们开发了一种有效的方法,用于模拟可激励单元的离子电流分量,该单元包含在未钳位电压下同时打开的数千个通道。通过使用二项分布的随机数将单通道打开-关闭随机事件合并到模型中。我们的模拟显示,在一个孤立的β细胞中,[Ca2 +] i会以较低的幅度振荡,而[Ca2 +] i则较低。然而,在紧密结合的细胞的大簇中,稳定的爆发发展,[Ca2 +] i随[Ca2 +] i的增加而以较大的幅度振荡。这可以解释为什么单个β细胞不会破裂并且也不会释放胰岛素。

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