A Novel Class of Cytochrome P450 Reductase Redox Cyclers: Cationic Manganoporphyrins

doi:10.1093/toxsci/kfi108

ToxSci Advance Access originally published online on February 9, 2005
Toxicological Sciences 2005 85(1):713-719; doi:10.1093/toxsci/kfi108

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Toxicological Sciences vol. 85 no. 1 © The Author 2005. Published by Oxford University Press on behalf of the Society of Toxicology. All rights reserved. For Permissions, please email: journals.permissions@oupjournals.org

A Novel Class of Cytochrome P450 Reductase Redox Cyclers: Cationic Manganoporphyrins

Brian J. Day^*^,^,^,1 and Chirag Kariya

^* Department of Medicine, National Jewish Medical & Research Center; Departments of Medicine and Pharmaceutical Sciences, University of Colorado Health Sciences Center, Denver, Colorado

Received December 9, 2004; accepted February 1, 2005

Manganese porphyrins are a potent class of catalytic antioxidantswhose activity was recently shown to be partially dependentupon flavin-containing enzymes (R. Kachadourian et al., 2004,Biochem. Pharmacol. 67, 77–85). We tested whether manganeseporphyrins could redox cycle with the flavin-containing enzyme,cytochrome P450 reductase, and whether this results in the inhibitionof xenobiotic metabolism. The effect of manganese porphyrinson xenobiotic metabolism in rat and human liver microsomes wasassessed spectrofluorometrically by following the O-dealkylationof benzyloxy- (BROD) and methoxyresorufin (MROD). Redox cyclingof manganese porphyrins with human cytochrome P450 reductasewas assessed both spectrophotometrically and polarographicallyby following the consumption of NADPH and oxygen, respectively.The tetrakis(N-pyridinium-2-yl) meso-substituted manganoporphyrin,MnTEPyP⁵⁺, and the tetrakis(1,3-dimethyl imidazolium-2-yl) meso-substitutedmanganoporphyrin, MnTDMIP⁵⁺, were 40 to 100 times more potentinhibitors of rat and human liver microsomal BROD metabolismthan the tetrakis(1,3-diethyl imidazolium-2-yl) meso-substitutedmanganoporphyrin, MnTDEIP⁵⁺, or the tetrakis(4-benzoic acid)meso-substituted manganoporphyrin, MnTBAP. A similar patternof inhibition was also seen in ß-naphthoflavone-inducedrat liver microsomal MROD metabolism. This pattern of xenobioticmetabolism inhibition correlated with the compound's abilityto redox cycle with cytochrome P450 reductase where MnTEPyP⁵⁺was more potent than MnTDEIP⁵⁺. Furthermore, redox cycling ofMnTEPyP⁵⁺ with cytochrome P450 reductase was inhibited by theflavin domain inhibitor diphenyleneiodonium. Small changes tothe carbon chain length on the imidazolium side groups had alarge effect on this activity. It is possible that interactionsbetween manganoporphyrins and flavin-dependent oxidoreductasescan account for both adverse and beneficial effects of the compounds.

Key Words: xenobiotic metabolism; catalytic antioxidants; oxidoreductase; human; rat.

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