| Literature DB >> 25650139 |
Raphael M Franzini1, Torun Ekblad, Nan Zhong, Moreno Wichert, Willy Decurtins, Angela Nauer, Mauro Zimmermann, Florent Samain, Jörg Scheuermann, Peter J Brown, Jonathan Hall, Susanne Gräslund, Herwig Schüler, Dario Neri.
Abstract
Methods for the rapid and inexpensive discovery of hit compounds are essential for pharmaceutical research and DNA-encoded chemical libraries represent promising tools for this purpose. We here report on the design and synthesis of DAL-100K, a DNA-encoded chemical library containing 103 200 structurally compact compounds. Affinity screening experiments and DNA-sequencing analysis provided ligands with nanomolar affinities to several proteins, including prostate-specific membrane antigen and tankyrase 1. Correlations of sequence counts with binding affinities and potencies of enzyme inhibition were observed and enabled the identification of structural features critical for activity. These results indicate that libraries of this type represent a useful source of small-molecule binders for target proteins of pharmaceutical interest and information on structural features important for binding.Keywords: combinatorial chemistry; drug discovery; encoded libraries; high-throughput screening; structure-activity relationships
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Year: 2015 PMID: 25650139 DOI: 10.1002/anie.201410736
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 15.336