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Development of a Selection Method for Discovering Irreversible (Covalent) Binders from a DNA-Encoded Library.


ABSTRACT: DNA-encoded libraries (DELs) have been broadly applied to identify chemical probes for target validation and lead discovery. To date, the main application of the DEL platform has been the identification of reversible ligands using multiple rounds of affinity selection. Irreversible (covalent) inhibition offers a unique mechanism of action for drug discovery research. In this study, we report a developing method of identifying irreversible (covalent) ligands from DELs. The new method was validated by using 3C protease (3CP) and on-DNA irreversible tool compounds (rupintrivir derivatives) spiked into a library at the same concentration as individual members of that library. After affinity selections against 3CP, the irreversible tool compounds were specifically enriched compared with the library members. In addition, we compared two immobilization methods and concluded that microscale columns packed with the appropriate affinity resin gave higher tool compound recovery than magnetic beads.

SUBMITTER: Zhu Z 

PROVIDER: S-EPMC7221453 | biostudies-literature | 2019 Feb

REPOSITORIES: biostudies-literature

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Development of a Selection Method for Discovering Irreversible (Covalent) Binders from a DNA-Encoded Library.

Zhu Zhengrong Z   Grady LaShadric C LC   Ding Yun Y   Lind Kenneth E KE   Davie Christopher P CP   Phelps Christopher B CB   Evindar Ghotas G  

SLAS discovery : advancing life sciences R & D 20181101 2


DNA-encoded libraries (DELs) have been broadly applied to identify chemical probes for target validation and lead discovery. To date, the main application of the DEL platform has been the identification of reversible ligands using multiple rounds of affinity selection. Irreversible (covalent) inhibition offers a unique mechanism of action for drug discovery research. In this study, we report a developing method of identifying irreversible (covalent) ligands from DELs. The new method was validate  ...[more]

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