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Verapamil metabolism in distinct regions of the heart and in cultures of cardiomyocytes of adult rats

 
: Walles, M.; Thum, T.; Levsen, K.; Borlak, J.

Drug metabolism and disposition 29 (2001), No.5, pp.761-768
ISSN: 0090-9556
English
Journal Article
Fraunhofer ITA ( ITEM) ()
CYP monooxygenase; Verapamil; metabolism; drug; side effect; oxidation; liquid chromatography; mass spectrometry; Cytochrome P-450

Abstract
A substantial number of drugs act either directly or indirectly on the heart, but surprisingly, little is known about drug oxidation in the heart. We therefore investigated the metabolism of the calcium antagonist verapamil in microsomal fractions isolated from the left and right ventricle of heart muscle and in primary cultures of cardiomyocytes of adult rats. Metabolism of verapamil proceeded predominantly with microsomal fractions isolated from the right ventricle of rat heart, and in liquid chromatographic-tandem mass spectrometry (LC-MS/MS) and LC-MS(3) experiments four metabolites (M1-M4) could be identified. Furthermore, the intermediate biotransformation products M5 to M8 could additionally be identified in cultures of primary cardiomyocytes, thus providing new insight into the mechanisms of the N-dealkylation and O-demethylation pathway of verapamil. We show metabolism of verapamil to be predominant in the right ventricle of the heart, and the data reported herein may explain metabolic inactivation and/or adverse drug reactions of certain cardiovascular drugs on the basis of tissue specific metabolism.

: http://publica.fraunhofer.de/documents/N-9229.html