Inhibition of ethoxy- and pentoxy-resorufin dealkylases of rat liver by flavones and flavonols: structure-activity relationship
- 1 July 1989
- journal article
- conference paper
- Published by Springer Nature in European Journal of Drug Metabolism and Pharmacokinetics
- Vol. 14 (3), 235-239
- https://doi.org/10.1007/bf03190104
Abstract
Summary The inhibitory effects of 17 flavones and flavonols on ethoxy- and pentoxy-resorufin dealkylases of rat liver were investigated. Several findings concerning the relationship between structure and activity can be pointed out The presence or lack of hydroxyl groups on the Havane nucleus has no influence on the efficiency of inhibition. Flavone and quercetin result in the same degree of inhibition. For polyhydroxylated molecules, the position of hydroxyl groups on A and B rings was an important factor. The more powerful inhibitors were the flavones having hydroxyl groups only on the A ring (e.g. chrysin) and the inhibitory effect was decreased by addition of hydroxyl substituents on the B group (e.g. quercetin). EROD activities were more responsive than PROD activities. Flavone and quercetin were competitive inhibitors of EROD activity whereas chrysin and morin were mixed type inhibitors. In the case of PROD activity, all four flavones were of the mixed type inhibitors.Keywords
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