Novel irreversible covalent BTK inhibitors discovered using DNA-encoded chemistry

Libraries of DNA-Encoded small molecules created using combinatorial chemistry and synthetic oligonucleotides are being applied to drug discovery projects across the pharmaceutical industry. The majority of reported projects describe the discovery of reversible, i.e. non-covalent, target modulators. We synthesized multiple DNAencoded chemical libraries terminated in electrophiles and then used them to discover covalent irreversible inhibitors and report the successful discovery of acrylamide- and epoxide-terminated Bruton's Tyrosine Kinase (BTK) inhibitors. We also demonstrate their selectivity, potency and covalent cysteine engagement using a range of techniques including X-ray crystallography, thermal transition shift assay, reporter displacement assay and intact protein complex mass spectrometry. The epoxide BTK inhibitors described here are the first ever reported to utilize this electrophile for this target.

Novel irreversible covalent BTK inhibitors discovered using DNA-encoded chemistry

Generating macrocyclic inhibitors of protein-protein interactions

Identification of broad anti-coronavirus chemical agents for repurposing against SARS-CoV-2 and variants of concern

m6A methylation potentiates cytosolic dsDNA recognition in a sequence-specific manner

Generating macrocyclic inhibitors of protein-protein interactions

Identification of broad anti-coronavirus chemical agents for repurposing against SARS-CoV-2 and variants of concern

m6A methylation potentiates cytosolic dsDNA recognition in a sequence-specific manner