Screening a fragment cocktail library using ultrafiltration

Sayaka Shibata,Zhongsheng Zhang,Konstantin V. Korotkov,Jaclyn R. Delarosa,Alberto J. Napuli,Angela Kelley,Natasha Mueller,Jennifer M. Ross,Frank Zucker,Frederick S. Buckner,Ethan A. Merritt,Christophe L. M. J. Verlinde,Wesley C. Van Voorhis,Wim G. J. Hol,Erkang Fan

Screening a fragment cocktail library using ultrafiltration

2011

Sayaka Shibata
Zhongsheng Zhang
Konstantin V. Korotkov
Jaclyn R. Delarosa
Alberto J. Napuli
Angela Kelley
Natasha Mueller
Jennifer M. Ross
Frank Zucker
Frederick S. Buckner
Ethan A. Merritt
Christophe L. M. J. Verlinde
Wesley C. Van Voorhis
Wim G. J. Hol
Erkang Fan

Ultrafiltration provides a generic method to discover ligands for protein drug targets with millimolar to micromolar Kd, the typical range of fragment-based drug discovery. This method was tailored to a 96-well format, and cocktails of fragment-sized molecules, with molecular masses between 150 and 300 Da, were screened against medical structural genomics target proteins. The validity of the method was confirmed through competitive binding assays in the presence of ligands known to bind the target proteins.

Keywords:

Drug
Fragment-based lead discovery
Combinatorial chemistry
Drug discovery
Ultrafiltration
Plasma protein binding
Structural genomics
Chemistry
Ligand
Small Molecule Libraries
competitive binding

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