Capillary-driven microchip integrated with nickel phosphide hybrid-modified electrode for the electrochemical detection of glucose.

BACKGROUND: Transition metal phosphides with properties similar to platinum metal have received increasing attention for the non-enzymatic detection of glucose. However, the requirement of highly corrosive reagent during sample pretreatment would impose a potential risk to the human body, limiting their practical applications. RESULTS: In this study, we report a self-powered microfluidic device for the non-enzymatic detection of glucose using nickel phosphide (Ni2P) hybrid as the catalyst. The Ni2P hybrid is synthesized by pyrolysis of metal-organic framework (MOF)-based precursor and in-situ phosphating process, showing two linear detection ranges (1 µM-1 mM, 1 mM-6 mM) toward glucose with the detection limit of 0.32 µM. The good performance of Ni2P hybrid for glucose is attributed to the synergistic effect of Ni2P active sites and N-doped porous carbon matrix. The microchip is integrated with a NaOH-loaded paper pad and a capillary-based micropump, enabling the automatic NaOH redissolution and delivery of sample solution into the detection chamber. Under the optimized condition, the Ni2P hybrid-based microchip realized the detection of glucose in a user-friendly way. Besides, the feasibility of using this microchip for glucose detection in real serum samples has also been validated. SIGNIFICANCE: This article presents a facile fabrication method utilizing a MOF template to synthesize a Ni2P hybrid catalyst. By leveraging the synergy between the Ni2P active sites and the N-doped carbon matrix, an exceptional electrochemical detection performance for glucose has been achieved. Additionally, a self-powered chip device has been developed for convenient glucose detection based on the pre-established high pH environment on the chip.

Synthesis of cobalt phosphide hybrid for simultaneous electrochemical detection of ascorbic acid, dopamine, and uric acid.

Ascorbic acid (AA), dopamine (DA), and uric acid (UA) are important biomarkers for the clinical screening of diseases. However, the simultaneous determination of these three analytes is still challenging. Herein, we report a facile metal-organic framework (MOF)-derived method to synthesize a cobalt phosphide (Co2P) hybrid for the simultaneous electrochemical detection of AA, DA and UA. The introduction of highly dispersed Co2P nanoparticles onto a P, N-doped porous carbon matrix is responsible for providing abundant active sites and facilitating electron transfer, thereby contributing to the improved electrocatalytic performance of the hybrid. Well-resolved oxidation peaks and an enhanced current response for the simultaneous oxidation of AA, DA, and UA were achieved using a Co2P hybrid-modified screen-printed electrode (Co2P hybrid-SPE) with the differential pulse voltammetry (DPV) method. The detection limits for AA, DA, and UA in simultaneous detection were calculated as 17.80 µM, 0.018 µM, and 0.068 µM (S/N = 3), respectively. Furthermore, the feasibility of using Co2P hybrid-SPE for the simultaneous detection of AA, DA, and UA in real serum samples was also confirmed.