Affiliation:
1. Wyeth Research Division of Biological Chemistry 401 N. Middletown Road Pearl River, NY 10965,
Abstract
For the development of fluorescence polarization (FP) competition assays, there is a widespread belief that tight-binding fluorescent ligands should be avoided to identify inhibitors of low or intermediate potency in the screening of small-molecule compound libraries. It is demonstrated herein that this statement is a misconception; in fact, the higher the affinity of the fluorescent ligand, the wider the range of inhibitor potency that can be resolved. An approximate estimate for the low end of inhibitor Ki values that can be resolved is the Kd value of the fluorescent ligand. Because FP competition assays are typically conducted under nonstoichiometric titration conditions, it is suggested that a fluorescent ligand of highest affinity that also has an adequate quantum yield to satisfy such conditions be selected. ( Journal of Biomolecular Screening 2003:34-38)
Cited by
172 articles.
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