4.5 Article

Continuous Glucose Monitoring in Hypoxic Environments Based on Water Splitting-Assisted Electrocatalysis

Journal

CHEMOSENSORS
Volume 11, Issue 2, Pages -

Publisher

MDPI
DOI: 10.3390/chemosensors11020149

Keywords

nonenzymatic; glucose; sensor; interstitial fluid; hypoxia

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Conventional enzyme-based glucose sensors using dissolved oxygen as the electron-transfer mediator may cause biased detection results, affect sensor response, and compromise long-term stability due to fluctuation of oxygen and continuous production of corrosive hydrogen peroxide. In this study, we introduce an oxygen-independent nonenzymatic glucose sensor based on water splitting-assisted electrocatalysis, which shows acceptable sensitivity, reliability, and biocompatibility for continuous glucose monitoring in hypoxic environments. This technique holds promise for monitoring glucose in clinically hypoxic patients.
Conventional enzyme-based continuous glucose sensors in interstitial fluid usually rely on dissolved oxygen as the electron-transfer mediator to bring electrons from oxidase to electrode while generating hydrogen peroxide. This may lead to several problems. First, the sensor may provide biased detection results owing to fluctuation of oxygen in interstitial fluid. Second, the polymer coatings that regulate the glucose/oxygen ratio can affect the dynamic response of the sensor. Third, the glucose oxidation reaction continuously produces corrosive hydrogen peroxide, which may compromise the long-term stability of the sensor. Here, we introduce an oxygen-independent nonenzymatic glucose sensor based on water splitting-assisted electrocatalysis for continuous glucose monitoring. For the water splitting reaction (i.e., hydrogen evolution reaction), a negative pretreatment potential is applied to produce a localized alkaline condition at the surface of the working electrode for subsequent nonenzymatic electrocatalytic oxidation of glucose. The reaction process does not require the participation of oxygen; therefore, the problems caused by oxygen can be avoided. The nonenzymatic sensor exhibits acceptable sensitivity, reliability, and biocompatibility for continuous glucose monitoring in hypoxic environments, as shown by the in vitro and in vivo measurements. Therefore, we believe that it is a promising technique for continuous glucose monitoring, especially for clinically hypoxic patients.

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