Flavonoid Derivatives as Adenosine Receptor Antagonists: A Comparison of the Hypothetical Receptor Binding Site Based on a Comparative Molecular Field Analysis Model

Abstract

Flavonoid derivatives have been optimized as relatively rigid antagonists of adenosine receptors with particular selectivity for the A₃ receptor subtype. A quantitative study of the structure-activity relationships for binding of flavonoids to adenosine A₁, A_2A, and A₃ receptors has been conducted using comparative molecular field analysis (CoMFA). Correlation coefficients (cross-validated r²) of 0.605, 0.595, and 0.583 were obtained for the three subtypes, respectively. All three CoMFA models have the same steric and electrostatic contributions, implying similar requirements inside the binding cavity. Similarities were seen in the topology of steric and electrostatic regions with the A₁ and A₃ receptors, but not the A_2A. Substitutions on the phenyl ring at the C-2 position of the chromone moiety may be considered important for binding affinity at all adenosine receptors. In the A₃ model a region of favorable bulk interaction is located around the 2‘-position of the phenyl ring. The presence of a C-6 substituent in the chromone moiety is well tolerated and increases the A₁/A₃ selectivity. The CoMFA coefficient contour plots provide a self-consistent picture of the main chemical features responsible for the pK_i variations and also result in predictions which agree with experimental values.