Covalent drug discovery using sulfur(VI) fluoride exchange warheads
- PMID: 37243622
- DOI: 10.1080/17460441.2023.2218642
Covalent drug discovery using sulfur(VI) fluoride exchange warheads
Abstract
Introduction: Covalent drug discovery has traditionally focused on targeting cysteine, but the amino acid is often absent in protein binding sites. This review makes the case to move beyond cysteine labeling using sulfur (VI) fluoride exchange (SuFEx) chemistry to expand the druggable proteome.
Areas covered: Recent advances in SuFEx medicinal chemistry and chemical biology are described, which have enabled the development of covalent chemical probes that site-selectively engage amino acid residues (including tyrosine, lysine, histidine, serine, and threonine) in binding pockets. Areas covered include chemoproteomic mapping of the targetable proteome, structure-based design of covalent inhibitors and molecular glues, metabolic stability profiling, and synthetic methodologies that have expedited the delivery of SuFEx modulators.
Expert opinion: Despite recent innovations in SuFEx medicinal chemistry, focused preclinical research is required to ensure the field moves from early chemical probe discovery to the delivery of transformational covalent drug candidates. The authors believe that covalent drug candidates designed to engage residues beyond cysteine using sulfonyl exchange warheads will likely enter clinical trials in the coming years.
Keywords: SuFEx; Sulfonyl fluoride; chemoproteomics; fluorosulfate; sulfuramidimidoyl fluoride; targeted covalent inhibitor, electrophilic warhead.
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