Single Drop Electroanalysis and Interfacial Interactions: Sensitivity versus Limit of Detection†.

Abstract

We report single drop electroanalytical measurements of pharmaceutically and biologically relevant compounds using screen printed electrodes (SPEs) modified with carboxylated multiwalled carbon nanotubes (MWCNT-COOH) as the sensor surface. Acetaminophen, nicotine, ascorbic acid, and nicotinamide adenine dinucleotide reduced form (NADH) were detected in a single drop of solution. We show that combined polar and nonpolar interactions of analytes with -COOH functional groups and large surface area of MWCNT, respectively, allow highly sensitive analyte detection with wide dynamic range. Smaller analytes can bind to a significantly greater number of sensor sites than the bulkier analytes and offer better detection sensitivity. Results suggest that sensitivity is controlled by predominant nonpolar interactions that an analyte can undergo with the MWCNT-COOH SPE sensor surface, whereas limit of detection is controlled by the extent of polar interactions between an analyte and the sensor surface, facilitating interfacial charge transport and an electrochemical signal output. Furthermore, a combination of polar and nonpolar analyte interactions with the sensor surface shows a synergistic effect on sensitivity and detection limit. This could be a likely reason for why sensitivity does not need to always correlate with lower detection limits as variations in the interfacial interactions are critical. Application of the designed single drop method to real samples was validated by estimating the amounts of acetaminophen, nicotine, ascorbic acid, and NADH in commercially available pharmaceuticals with excellent recovery.