Mixed host co-assembled systems for broad-scope analyte sensing

29 February 2024, Version 1
This content is a preprint and has not undergone peer review at the time of posting.

Abstract

Here we report a systems-oriented approach to developing information-rich mixed host chemosensors. We show that co-assembling macro-cyclic hosts from different classes, DimerDye sulfonatocalix[4]arenes and cucurbit[n]urils, effectively increases the scope of analyte binding interactions and therefore, sensory outputs. This simple dynamic strategy exploits cross-reactive noncovalent host-host complexation interactions while integrating a reporter dye, thereby producing emergent photophysical responses when an analyte interacts with either host. We first demonstrate the advantages of mixed host co-assembled chemosensors through an increased detection range of hydrophobic, cationic, neutral, and anionic drugs. We then implement mixed host sensors in an array-based platform for the differentiation of illicit drugs, including cannabinoids, benzodiazepine analogs, opiates, anesthetics, amphetamine, and common adulterating substances. Finally, the potential of this approach is applied to profiling real-world multi-component illicit street drug samples, proving to be more effective than classical sensor arrays.

Supplementary materials

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Description
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PCA Raw Data
Description
Absorbance and fluorescence responses used in PCA analysis of drug analytes and multi-component drug samples
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