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Journal Article
Mar, 2026

A unified platform for nucleoside analog synthesis

Matthew J. Anketell, Ethan Fung, Wenbin Liu, Mahesh Shinde, Cyndi Qixin He, Kurtis W. C. Ng, Steven M. Silverman, Louis-Charles Campeau, Ralph Pantophlet, Robert Britton

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DOI: 10.1126/science.aed6880
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Abstract

Nucleoside analogs (NAs) are essential as antiviral and anticancer therapies. Despite decades of focused medicinal chemistry efforts, their related chemical space remains underexplored, mainly owing to their lengthy, single-molecule–oriented syntheses that lack the flexibility required to generate NA libraries. Here we report a flexible, robust, and efficient platform for the high-throughput synthesis of NAs using a photoredox coupling strategy. This approach produces both carbon- and nitrogen-linked NAs and unifies the synthesis of several disparate NA classes, including 4′-thio, 4′-imino, and ProTides, all from a simple, scalable intermediate. Using this platform, we demonstrate the production of a diverse NA library and identify several hit compounds with anti–HIV-1 activity. We expect that this newly developed approach to NAs will inspire and support drug discovery efforts in this area.

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    Date of publication: 5 Mar, 2026Number of views: 14
    Full text: www.science.org
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    Matthew J. Anketell et al. ,A unified platform for nucleoside analog synthesis.Science392,eaed6880(2026).DOI:10.1126/science.aed6880

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    392, №6799

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