| Literature DB >> 33833446 |
Nicholas Favalli1, Gabriele Bassi1, Christian Pellegrino1, Jacopo Millul2, Roberto De Luca2, Samuele Cazzamalli2, Su Yang3, Anika Trenner4, Nour L Mozaffari4, Renier Myburgh5, Mustafa Moroglu6, Stuart J Conway6, Alessandro A Sartori4, Markus G Manz5, Richard A Lerner7, Peter K Vogt3, Jörg Scheuermann8, Dario Neri9.
Abstract
The encoding of chemical compounds with amplifiable DNA tags facilitates the discovery of small-molecule ligands for proteins. To investigate the impact of stereo- and regiochemistry on ligand discovery, we synthesized a DNA-encoded library of 670,752 derivatives based on 2-azido-3-iodophenylpropionic acids. The library was selected against multiple proteins and yielded specific ligands. The selection fingerprints obtained for a set of protein targets of pharmaceutical relevance clearly showed the preferential enrichment of ortho-, meta- or para-regioisomers, which was experimentally verified by affinity measurements in the absence of DNA. The discovered ligands included novel selective enzyme inhibitors and binders to tumour-associated antigens, which enabled conditional chimeric antigen receptor T-cell activation and tumour targeting.Entities:
Year: 2021 PMID: 33833446 DOI: 10.1038/s41557-021-00660-y
Source DB: PubMed Journal: Nat Chem ISSN: 1755-4330 Impact factor: 24.427