Yu Zhou scite author profile

Dynamic combinatorial library (DCL) has emerged as an efficient tool for ligand discovery and become an important discovery modality in biomedical research. However, the applications of DCLs have been significantly hampered by low library diversity and limited analytical methods capable of processing large libraries. Here, we report a strategy that has addressed this limitation and can select cooperatively binding small-molecule pairs from large-scale dynamic libraries. Our approach is based on DNA-mediated dynamic hybridization, DNA-encoding, and a photo-crosslinking-based decoding scheme. To demonstrate the generality and performance of this approach, a 10 000-member DNAencoded dynamic library has been prepared and selected against six protein targets. Specific binders have been identified for each target, and we have validated the biological activities of selected ligands for the targets that are implicated in important cellular functions including protein deacetylation and sumoylation. Notably, a series of novel and selective sirtuin-3 inhibitors have been developed. Our study has circumvented a major obstacle in DCL and may provide a broadly applicable method for ligand discovery against biological targets.

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Future challenges with DNA-encoded chemical libraries in the drug discovery domain

Zhao

Huang

Zhou

et al. 2019

Expert Opinion on Drug Discovery

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Yu Zhou

Selection of DNA-encoded chemical libraries against endogenous membrane proteins on live cells

DNA-Encoded Dynamic Chemical Library and Its Applications in Ligand Discovery

Future challenges with DNA-encoded chemical libraries in the drug discovery domain

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