Title of article
Enhanced Ligand Affinity for Receptors in which Components of the Binding Site Are Independently Mobile Original Research Article
Author/Authors
Clare R. Trevitt، نويسنده , , C. Jeremy Craven، نويسنده , , Lilia Milanesi، نويسنده , , Karl Syson، نويسنده , , Maija-Liisa Mattinen، نويسنده , , Julie Perkins، نويسنده , , Arto Annila، نويسنده , , Christopher A. Hunter، نويسنده , , Panos Soultanas and Jonathan P. Waltho، نويسنده ,
Issue Information
ماهنامه با شماره پیاپی سال 2005
Pages
9
From page
89
To page
97
Abstract
Using calmodulin antagonism as a model, it is demonstrated that, under circumstances in which binding sites are motionally independent, it is possible to create bifunctional ligands that bind with significant affinity enhancement over their monofunctional counterparts. Suitable head groups were identified by using a semiquantitative screen of monofunctional tryptophan analogs. Two bifunctional ligands, which contained two copies of the highest-affinity head group tethered by rigid linkers, were synthesized. The bifunctional ligands bound to calmodulin with a stoichiometry of 1:1 and with an affinity enhancement over their monofunctional counterparts; the latter bound with a stoichiometry of 2:1 ligand:protein. A lower limit to the effective concentrations of the domains of calmodulin relative to each other (0.2–2 mM) was determined. A comparable effective concentration was achieved for bifunctional ligands based on higher-affinity naphthalene sulphonamide derivatives.
Journal title
Chemistry and Biology
Serial Year
2005
Journal title
Chemistry and Biology
Record number
1158972
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