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微流控检测与多模态钙离子信号动力学的数学建模。

Microfluidic interrogation and mathematical modeling of multi-regime calcium signaling dynamics.

机构信息

Biomedical Engineering Department, University of Michigan, Gerstacker Building, 2200 Bonisteel Blvd, Ann Arbor, MI 48109, USA.

出版信息

Integr Biol (Camb). 2013 Jul 24;5(7):932-9. doi: 10.1039/c3ib40032h. Epub 2013 Jun 4.

Abstract

Through microfluidic interrogation we analyzed real-time calcium responses of HEK293 cells stimulated with short pulses of the M3 muscarinic receptor ligand carbachol in two different concentration regimes. Lower ligand concentrations elicit oscillatory calcium signals while higher concentrations trigger a rapid rise that eventually settles down at a steady-state slightly above pre-stimulus levels, referred to as an acute signal. Cells were periodically pulsed with carbachol at these two concentration regimes using a custom-made microfluidic platform, and the resulting calcium signals were measured with a single fluorescent readout. Pulsed stimulations at these two concentration regimes resulted in multiple types of response patterns that each delivered complementary information about the M3 muscarinic receptor signaling pathway. These multiple types of calcium response patterns enabled development of a comprehensive mathematical model of multi-regime calcium signaling. The resulting model suggests that dephosphorylation of deactivated receptors is rate limiting for recovery of calcium signals in the acute regime (high ligand concentration), while calcium replenishment and IP3 production determine signal recovery in the oscillatory regime (low ligand concentration). This study not only provides mechanistic insight into multi-regime signaling of the M3 muscarinic receptor pathway, but also provides a general strategy for analyzing multi-regime pathways using only one fluorescent readout.

摘要

通过微流控检测,我们分析了 HEK293 细胞在两种不同浓度下受到 M3 毒蕈碱受体配体乙酰甲胆碱短脉冲刺激时的实时钙反应。较低的配体浓度会引起钙信号的振荡,而较高的浓度则会引发迅速上升,最终在略高于刺激前水平的稳定状态下稳定下来,称为急性信号。我们使用定制的微流控平台在这两种浓度下周期性地对细胞进行乙酰甲胆碱脉冲刺激,并通过单次荧光读取来测量由此产生的钙信号。在这两种浓度下进行的脉冲刺激产生了多种类型的反应模式,每种模式都提供了关于 M3 毒蕈碱受体信号通路的补充信息。这些多种类型的钙反应模式使我们能够开发出一种全面的多模式钙信号数学模型。该模型表明,在急性阶段(高配体浓度),失活受体的去磷酸化是钙信号恢复的限速步骤,而钙补充和 IP3 产生则决定了振荡阶段(低配体浓度)信号的恢复。这项研究不仅为 M3 毒蕈碱受体途径的多模式信号提供了机制上的见解,还为仅使用一种荧光读取来分析多模式途径提供了一种通用策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bd65/3704220/66406c0a5d5f/nihms488608f1.jpg

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