Human cytosolic enzymes involved in the metabolic activation of carcinogenic aristolochic acid: evidence for reductive activation by human NAD(P)H:quinone oxidoreductase

doi:10.1093/carcin/bgg119

Carcinogenesis Advance Access originally published online on July 17, 2003

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Carcinogenesis, Vol. 24, No. 10, 1695-1703, October 2003
© 2003 Oxford University Press

CARCINOGENESIS

Human cytosolic enzymes involved in the metabolic activation of carcinogenic aristolochic acid: evidence for reductive activation by human NAD(P)H:quinone oxidoreductase

Marie Stiborová¹^,3, Eva Frei², Bruno Sopko¹, Klára Sopková¹, Vladimíra Marková¹, Martina La $n$ ková¹, Tereza Kumst $y$ $r$ ová¹, Manfred Wiessler² and Heinz H. Schmeiser²

¹ Department of Biochemistry, Faculty of Science, Charles University, Albertov 2030, 128 40 Prague 2, The Czech Republic and ² Division of Molecular Toxicology, German Cancer Research Center, Im Neuenheimer Feld 280, D-69120 Heidelberg, Germany

Aristolochic acid (AA), a naturally occurring nephrotoxin andcarcinogen, has been associated with the development of urothelialcancer in humans. Understanding which human enzymes are involvedin AA metabolism is important in the assessment of an individual'ssusceptibility to this carcinogen. Using the ³²P-postlabelingassay we examined the ability of enzymes of cytosolic samplesfrom 10 different human livers and from one human kidney toactivate the major component of the plant extract AA, 8-methoxy-6-nitro-phenanthro-(3,4-d)-1,3-dioxolo-5-carboxylic acid (AAI),to metabolites forming adducts in DNA. Cytosolic fractions ofboth organs generated AAI–DNA adduct patterns reproducingthose found in renal tissues from humans exposed to AA. 7-(Deoxyadenosin-N⁶-yl)aristolactamI, 7-(deoxyguanosin-N²-yl)aristolactam I and 7-(deoxyadenosin-N⁶-yl)aristolactamII, indicating a possible demethoxylation reaction of AAI, wereidentified as AA–DNA adducts formed from AAI by all humanhepatic and renal cytosols. To define the role of human cytosolicreductases in the activation of AAI, we investigated the modulationof AAI–DNA adduct formation by cofactors or selectiveinhibitors of the NAD(P)H:quinone oxidoreductase (NQO1), xanthineoxidase (XO) and aldehyde oxidase. We also determined whetherthe activities of NQO1 and XO in different human hepatic cytosolicsamples correlated with the levels of AAI–DNA adductsformed by the same cytosolic samples. Based on these studies,we attribute most of the activation of AA in human cytosolsto NQO1, although a role of cytosolic XO cannot be ruled out.With purified NQO1 from rat liver and kidney and XO from buttermilk,the major role of NQO1 in the formation of AAI–DNA adductswas confirmed. The orientation of AAI in the active site ofhuman NQO1 was predicted from molecular modeling based on publishedX-ray structures. The results demonstrate for the first timethe potential of human NQO1 to activate AAI by nitroreduction.

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