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首页> 外文期刊>Analytical chemistry >Development and Application of a Self-Referencing Glucose Microsensor for the Measurement of Glucose Consumption by Pancreatic β-Cells
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Development and Application of a Self-Referencing Glucose Microsensor for the Measurement of Glucose Consumption by Pancreatic β-Cells

机译:自参考型葡萄糖微传感器在胰腺β细胞测量葡萄糖消耗中的开发与应用

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Glucose gradients generated by an artificial source and β-cells were measured using an enzyme-based glucose microsensor, 8-μm tip diameter, as a self-referencing electrode. The technique is based on a difference measurement between two locations in a gradient and thus allows us to obtain real-time flux values with minimal impact of sensor drift or noise. Flux values were derived by incorporation of the measured differential current into Fick's first equation. In an artificial glucose gradient, a flux detection limit of 8.2±0.4 pmol·cm~(-2)·s~(-1) (mean±SEM, n=7) with a sensor sensitivity of 7.0±0.4 pA/mM (mean±SEM, n=16) was demonstrated. Under biological conditions, the glucose sensor showed no oxygen dependence with 5 mM glucose in the bulk medium. The addition of catalase to the bulk medium was shown to ameliorate surface-dependent flux distortion close to specimens, suggesting an underlying local accumulation of hydrogen peroxide. Glucose flux from β-cell clusters, measured in the presence of 5 mM glucose, was 61.7±9.5 fmol·nL~(-1)·s~(-1) (mean±SEM, n=9) and could be pharmacologically modulated. Glucose consumption in response to FCCP (1 μM) transiently increased, subsequently decreasing to below basal by 93±16 and 56±6%, respectively (mean±SEM, n=5). Consumption was decreased after the application of 10 μM rotenone by 74±5% (mean±SEM, n=4). These results demonstrate that an enzyme-based amperometric microsensor can be applied in the self-referencing mode. Further, in obtaining glucose flux measurements from small clusters of cells, these are the first recordings of the real-time dynamic of glucose movements in a biological microenvironment.
机译:人工来源和β细胞产生的葡萄糖梯度使用基于酶的葡萄糖微传感器(尖端直径为8μm)作为自参考电极进行测量。该技术基于梯度中两个位置之间的差异测量,因此使我们能够在传感器漂移或噪声影响最小的情况下获得实时通量值。通过将测得的差分电流合并到Fick的第一个方程中,得出磁通值。在人造葡萄糖梯度中,通量检测极限为8.2±0.4 pmol·cm〜(-2)·s〜(-1)(平均值±SEM,n = 7),传感器灵敏度为7.0±0.4 pA / mM(平均值±SEM,n = 16)。在生物条件下,葡萄糖传感器在大体积培养基中对5 mM葡萄糖无氧依赖性。向过大的培养基中添加过氧化氢酶可改善与样品接近的表面依赖性通量畸变,表明潜在的过氧化氢局部积累。在5 mM葡萄糖存在下测得的来自β细胞簇的葡萄糖通量为61.7±9.5 fmol·nL〜(-1)·s〜(-1)(平均值±SEM,n = 9)并且可以进行药理调节。响应FCCP(1μM)的葡萄糖消耗瞬时增加,随后分别降至基础以下93±16和56±6%(平均值±SEM,n = 5)。施用10μM鱼藤酮后,消费量降低了74±5%(平均值±SEM,n = 4)。这些结果表明,可以在自参考模式下应用基于酶的电流微传感器。此外,在从小细胞簇中获得葡萄糖通量测量值时,这些是生物微环境中葡萄糖运动实时动态的第一笔记录。

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