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IN-VITRO CYTOCHROME-P450 MONOOXYGENASE AND PROSTAGLANDIN H-SYNTHASE MEDIATED AFLATOXIN-B(1) BIOTRANSFORMATION IN GUINEA-PIG TISSUES - EFFECTS OF BETA-NAPHTHOFLAVONE TREATMENT

被引:14
作者
LIU, L
NAKATSU, K
MASSEY, TE
机构
[1] QUEENS UNIV,DEPT PHARMACOL & TOXICOL,KINGSTON K7L 3N6,ONTARIO,CANADA
[2] QUEENS UNIV,DEPT MED,KINGSTON K7L 3N6,ONTARIO,CANADA
来源
ARCHIVES OF TOXICOLOGY | 1993年 / 67卷 / 06期
关键词
AFLATOXIN-B(1); CYTOCHROME-P450; PROSTAGLANDIN-H SYNTHASE; BETA-NAPHTHOFLAVONE; CHEMICAL CARCINOGENICITY;
D O I
10.1007/BF01977398
中图分类号
R99 [毒物学(毒理学)];
学科分类号
100405 ;
摘要
In the present study, we examined the effects of treating guinea pigs with beta-naphthoflavone (BNF) on aflatoxin B1 (AFB1) metabolism by microsomal cytochrome P450 monooxygenase (P450) and prostaglandin H synthase (PHS) in liver, lung and kidney tissues. After BNF treatment, microsomal 7-ethoxyresorufin 0-deethylase activity was induced 13-, 25- and 11-fold in lung, kidney and liver, respectively, confirming that the BNF treatment protocol was effective at inducing monooxygenase activity. Treatment of guinea pigs with BNF did not change [H-3]AFB1-DNA binding catalyzed by microsomal PHS or P450 in lung, kidney or liver. In contrast, AFM1 formation by P450 was significantly increased in microsomes from all three organs. The data indicate that BNF-inducible P450 isozymes of the P4501A class are responsible for the biotransformation of AFB1 to non-toxic metabolites. Guinea pig kidney microsomes could also catalyze NADPH-dependent formation of aflatoxicol (AFL), a metabolite usually produced by a cytosolic steroid dehydrogenase. Renal microsomal AFL formation was not altered by prior BNF treatment. The results in the present study suggest that BNF may alter the bioactivation of AFB1 in guinea pig tissues by inducing P450 activity, leading to the formation of less reactive metabolite.
引用
收藏
页码:379 / 385
页数:7
相关论文
共 43 条
[1]  
ADAMS RLP, 1986, BIOCH NUCL ACIDS, P459
[2]   ACTIVITY, INTRACELLULAR DISTRIBUTION AND SOME PROPERTIES OF 17BETA-HYDROXY-C19-STEROID DEHYDROGENASES IN LIVER AND KIDNEY [J].
AOSHIMA, Y ;
KOCHAKIAN, CD .
ENDOCRINOLOGY, 1963, 72 (01) :106-&
[3]   AFLATOXIN-B1 CARCINOGENESIS AND ITS RELATION TO DNA ADDUCT FORMATION AND ADDUCT PERSISTENCE IN SENSITIVE AND RESISTANT SALMONID FISH [J].
BAILEY, GS ;
WILLIAMS, DE ;
WILCOX, JS ;
LOVELAND, PM ;
COULOMBE, RA ;
HENDRICKS, JD .
CARCINOGENESIS, 1988, 9 (11) :1919-1926
[4]   PROSTAGLANDIN-H SYNTHASE-DEPENDENT EPOXIDATION OF AFLATOXIN B-1 [J].
BATTISTA, JR ;
MARNETT, LJ .
CARCINOGENESIS, 1985, 6 (08) :1227-1229
[5]  
BOYD JA, 1987, CANCER RES, V47, P4007
[6]   SELECTIVE G-MUTATION TO T-MUTATION OF P53 GENE IN HEPATOCELLULAR-CARCINOMA FROM SOUTHERN AFRICA [J].
BRESSAC, B ;
KEW, M ;
WANDS, J ;
OZTURK, M .
NATURE, 1991, 350 (6317) :429-431
[7]   ETHOXYPHENOXAZONES, PENTOXYPHENOXAZONES, AND BENZYLOXYPHENOXAZONES AND HOMOLOGS - A SERIES OF SUBSTRATES TO DISTINGUISH BETWEEN DIFFERENT INDUCED CYTOCHROMES-P-450 [J].
BURKE, MD ;
THOMPSON, S ;
ELCOMBE, CR ;
HALPERT, J ;
HAAPARANTA, T ;
MAYER, RT .
BIOCHEMICAL PHARMACOLOGY, 1985, 34 (18) :3337-3345
[8]   MODULATION OF AFLATOXIN-B1 BIOTRANSFORMATION IN RABBIT PULMONARY AND HEPATIC MICROSOMES [J].
DANIELS, JM ;
MASSEY, TE .
TOXICOLOGY, 1992, 74 (01) :19-32
[9]   BIOTRANSFORMATION OF AFLATOXIN-B1 IN RABBIT LUNG AND LIVER-MICROSOMES [J].
DANIELS, JM ;
LIU, L ;
STEWART, RK ;
MASSEY, TE .
CARCINOGENESIS, 1990, 11 (05) :823-827
[10]   ORAL SUBCUTANEOUS AND INTRATRACHEAL ADMINISTRATION OF CARCINOGENIC LACTONES AND RELATED SUBSTANCES - INTRATRACHEAL ADMINISTRATION OF CIGARETTE TAR IN RAT [J].
DICKENS, F ;
JONES, HEH ;
WAYNFORTH, HB .
BRITISH JOURNAL OF CANCER, 1966, 20 (01) :134-+
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