| Literature DB >> 36070343 |
Yunfei Cheng1, Gencheng Li1, Christopher J Smedley2, Marie-Claire Giel2, Seiya Kitamura1,3,4, Jordan L Woehl3, Giulia Bianco4, Stefano Forli4, Joshua A Homer5, John R Cappiello1, Dennis W Wolan3,4, John E Moses5, K Barry Sharpless1.
Abstract
Diversity Oriented Clicking (DOC) is a discovery method geared toward the rapid synthesis of functional libraries. It combines the best attributes of both classical and modern click chemistries. DOC strategies center upon the chemical diversification of core "SuFExable" hubs-exemplified by 2-Substituted-Alkynyl-1-Sulfonyl Fluorides (SASFs)-enabling the modular assembly of compounds through multiple reaction pathways. We report here a range of stereoselective Michael-type addition pathways from SASF hubs including reactions with secondary amines, carboxylates, 1H-1,2,3-triazole, and halides. These high yielding conjugate addition pathways deliver unprecedented β-substituted alkenyl sulfonyl fluorides as single isomers with minimal purification, greatly enriching the repertoire of DOC and holding true to the fundamentals of modular click chemistry. Further, we demonstrate the potential for biological function - a key objective of click chemistry - of this family of SASF-derived molecules as covalent inhibitors of human neutrophil elastase.Entities:
Keywords: Diversity Oriented Clicking; Michael addition; SuFEx; covalent inhibitor; human neutrophil elastase
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Year: 2022 PMID: 36070343 PMCID: PMC9478681 DOI: 10.1073/pnas.2208540119
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 12.779