Small Molecule Mitochondrial F1F0ATPase Hydrolase Inhibitors as Cardioprotective Agents. Identification of 4-(N-Arylimidazole)-Substituted Benzopyran Derivatives as Selective Hydrolase Inhibitors

Abstract

In this paper we show that 4-aryl-CH₂-imidazole-substituted benzopyran compounds with 3S,4R-stereochemistry are cardioprotective by inhibiting the F₁F₀ mitochondrial ATP hydrolase. Compounds (e.g., 13) with 3R,4S-stereochemistry act as mitochondrial K_ATP openers. This resulted from an inversion of stereochemistry for the F₁F₀ mitochondrial ATP hydrolase vs mitochondrial K_ATP. Structure−activity relationships for the inhibition of mitochondrial ATP hydrolase are also delineated. It is not clear how 13 (3R,4S) can selectively inhibit the hydrolytic activity of the F₁F₀ mitochondrial enzyme without interfering with the synthase activity.