AI Article Synopsis

  • A DNA-encoded library (DEL) aims to cover diverse chemical structures for effective drug discovery, but current methods for modifying less reactive phenols hinder progress in including useful chemotypes like diaryl ethers.
  • The study introduces a "substrate activation" strategy using diaryliodonium salts as electrophilic reagents to improve the selective arylation of DNA-bound phenols and oximes, achieving high yields while maintaining DNA integrity.
  • This innovative approach not only supports the late-stage modification of tyrosine-containing peptides but also facilitates the creation of DNA-tagged versions of existing drugs, enhancing the design and synthesis capabilities of DELs.

Article Abstract

A successful DNA-encoded library (DEL) will consist of diverse skeletons and cover chemical space as comprehensive as possible to fully realize its potential in drug discovery and chemical biology. However, the lack of versatile on-DNA arylation methods for phenols that are less nucleophilic and reactive poses a great hurdle for DEL to include diaryl ether, a privileged chemotype in pharmaceuticals and natural products. This work describes the use of "substrate activation" approach to address the arylation of DNA-conjugated phenols. Diaryliodonium salt, a highly electrophilic and reactive arylation reagent, is employed as Ar sources to ensure highly selective on-DNA arylation of phenols and oximes with both high yields and DNA fidelity. Notably, the new on-DNA arylation reaction can be applied to the late-stage modification of peptides containing tyrosine side-chain and to synthesize DNA-tagged analogues of existing drug molecules such as sorafenib, a known pan-kinase inhibitor. The new on-DNA diaryliodonium salts chemistry affords a greater flexibility in DEL design and synthesis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9475524PMC
http://dx.doi.org/10.1002/advs.202202790DOI Listing

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