Small Molecule Delivery in Living Cells by Gated Hydrolysis of Phosphinate Ester Dyes: Application to Acute Myeloid Leukemia

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

Abstract

Theranostic fluorescent platforms are capable of selective delivery of small molecules to target cells with simultaneous optical monitoring. Such technologies promise to significantly reduce off-target effects compared to cytotoxic chemotherapy. However, small molecule approaches are often hindered by relatively complex designs that are required to incorporate a fluorescent reporter, reactive linker, targeting ligand, and cargo into a single molecule. Herein, we provide the first direct evidence for the ability to gate the delivery of small molecule cargos from phosphinate ester-containing Nebraska Red (NR) dyes in vitro and in living cells. This simplified system integrates the fluorescent reporter, reactive linker, and targeting ligand into one species – a phosphinate ester dye. As a proof-of-principle for delivery of drug-like molecules to cells, we develop NR-HOCl-TFMU, which responds to hypochlorous acid (HOCl), a marker of acute myeloid leukemia (AML). NR-HOCl-TFMU is stable for days prior to reaction with HOCl, leading to phosphinate ester hydrolysis and production of a NIR (near-infrared, NR dye) and blue (cargo) fluorescent signal. NR dye fluorescence produced upon reaction with HOCl is directly proportional to cargo release, and NR-HOCl-TFMU is capable of selectively delivering its drug-like, small molecule cargo to AML cells in an HOCl-gated manner. In the long term, we envision the use of this technology to develop HOCl-gated cytotoxin delivery systems targeted towards AML cells. More broadly, this approach provides a potentially generalizable strategy for the development of simplified theranostic agents targeted towards small molecule analytes and enzymatic activities associated with disease.

Keywords

Drug Delivery
Theranostic
Functional Fluorophore
Fluorescent Probe

Supplementary materials

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