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Spatially Organized β-Cell Subpopulations Control Electrical Dynamics across Islets of Langerhans

机译:空间组织的β细胞亚群控制朗格汉斯岛上的电动力学

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摘要

Understanding how heterogeneous cells within a multicellular system interact and affect overall function is difficult without a means of perturbing individual cells or subpopulations. Here we apply optogenetics to understand how subpopulations of β-cells control the overall [Ca2+]i response and insulin secretion dynamics of the islets of Langerhans. We spatiotemporally perturbed electrical activity in β-cells of channelrhodopsin2-expressing islets, mapped the [Ca2+]i response, and correlated this with the cellular metabolic activity and an in silico electrophysiology model. We discovered organized regions of metabolic activity across the islet, and these affect the way in which β-cells electrically interact. Specific regions acted as pacemakers by initiating calcium wave propagation. Our findings reveal the functional architecture of the islet, and show how distinct subpopulations of cells can disproportionality affect function. These results also suggest ways in which other neuroendocrine systems can be regulated, and demonstrate how optogenetic tools can discern their functional architecture.
机译:如果不使用不干扰单个细胞或亚群的方法,则很难了解多细胞系统中的异种细胞如何相互作用并影响整体功能。在这里,我们使用光遗传学来了解β细胞亚群如何控制Langerhans胰岛的整体[Ca 2 + ] i反应和胰岛素分泌动力学。我们时空干扰表达通道视紫红质2的胰岛β细胞中的电活动,绘制[Ca 2 + ] i反应,并将其与细胞代谢活动和硅电生理模型相关联。我们发现了整个胰岛有组织的代谢活动区域,这些区域影响β细胞电相互作用的方式。特定区域通过启动钙波传播而充当起搏器。我们的发现揭示了胰岛的功能结构,并显示了不同的细胞亚群如何成比例地影响功能。这些结果还提出了可以调节其他神经内分泌系统的方式,并证明了光遗传学工具如何识别其功能结构。

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