METABOLISM OF AN IMIDAZOLE FUNGICIDE (PROCHLORAZ) IN THE RAT AFTER ORAL-ADMINISTRATION

被引：24

作者：

LAIGNELET, L ^{[1
]}

RIVIERE, JL ^{[1
]}

LHUGUENOT, JC ^{[1
]}

机构：

[1] ECOLE NATL VET LYON,ECOTOXICOL LAB,F-69280 MARCY LETOILE,FRANCE

来源：

FOOD AND CHEMICAL TOXICOLOGY | 1992年 / 30卷 / 07期

关键词：

D O I：

10.1016/0278-6915(92)90191-M

中图分类号：

TS2 [食品工业];

学科分类号：

0832 ;

摘要：

The metabolic fate and pathway of the imidazole fungicide prochloraz {1-[N-propyl-N-2-(2,4,6-trichlorophenoxy) ethyl carbamoyl] imidazole} were investigated in the rat after administration of oral single doses with radiolabelled molecules. At both dose levels (50 and 250 mg/kg body weight), virtually all of the ingested [C-14-phenyl]prochloraz was excreted in the urine or faeces within 96 hr, the bulk of excretion occurring between 24 and 48 hr after dosing. Urinary elimination accounted for 61 and 68% of the respective initial doses. Urinary metabolic products were isolated and identified by thin-layer chromatography, gas chromatography or gas chromatography coupled with mass spectrometry analysis. Prochloraz was completely metabolized with no unchanged compound being excreted in the urine. The main biotransformation products in rat urine were 2,4,6-trichlorophenoxyacetic acid and its corresponding alcohol, the latter as a glucuronic acid conjugate. Ring hydroxylation also occurred, with the hydroxy-2,4,6-trichlorophenoxyethanol and hydroxy-2,4,6-trichlorophenoxyacetic acid metabolites excreted in small amounts in the urine. 2,4,6-Trichlorophenol and unconjugated 2,4,6-trichlorophenoxyethanol were identified as minor urinary metabolites.

引用

页码：575 / 583

页数：9

共 24 条

[1] CHLOROPHENOXYACID HERBICIDES INDUCE MICROSOMAL CYTOCHROME-P-450 IVA1 (P-452) IN RAT-LIVER [J].

BACHER, MA ;

GIBSON, GG .

CHEMICO-BIOLOGICAL INTERACTIONS, 1988, 65 (02) :145-156

[2] EFFECTS OF STEROL BIOSYNTHESIS-INHIBITING (SBI) FUNGICIDES ON CYTOCHROME-P-450 OXYGENATIONS IN FUNGI [J].

HENRY, MJ ;

SISLER, HD .

PESTICIDE BIOCHEMISTRY AND PHYSIOLOGY, 1984, 22 (03) :262-275

[3] ENHANCED PEROXISOMAL BETA-OXIDATION OF FATTY-ACIDS AND GLUTATHIONE METABOLISM IN RATS EXPOSED TO PHENOXYACETIC ACIDS [J].

HIETANEN, E ;

AHOTUPA, M ;

HEINONEN, T ;

HAMALAINEN, H ;

KUNNAS, T ;

LINNAINMAA, K ;

MANTYLA, E ;

VAINIO, H .

TOXICOLOGY, 1985, 34 (02) :103-111

[4] EFFECTS OF 2,4-DICHLOROPHENOXYACETIC ACID AND 2,4,5-TRICHLOROPHENOXYACETIC ACID ON PEROXISOMAL ENZYMES IN RAT-LIVER [J].

KAWASHIMA, Y ;

KATOH, H ;

NAKAJIMA, S ;

KOZUKA, H ;

UCHIYAMA, M .

BIOCHEMICAL PHARMACOLOGY, 1984, 33 (02) :241-245

[5] GLUCURONIC ESTERS .4. SYNTHESIS OF 1-O-ACYL-D-GLUCOPYRANURONIC ACIDS VIA BENZYL 1-O-ACYL-2,3,4-TRI-O-BENZYL-D-GLUCOPYRANURONATES [J].

KEGLEVIC, D ;

PRAVDIC, N ;

TOMASIC, J .

JOURNAL OF THE CHEMICAL SOCIETY C-ORGANIC, 1968, (05) :511-&

[6] INDUCTION AND INHIBITION OF RAT-LIVER CYTOCHROME(S) P-450 BY AN IMIDAZOLE FUNGICIDE (PROCHLORAZ) [J].

LAIGNELET, L ;

NARBONNE, JF ;

LHUGUENOT, JC ;

RIVIERE, JL .

TOXICOLOGY, 1989, 59 (03) :271-284

[7] DEVELOPMENT OF HEPATOCELLULAR CARCINOMAS AND INCREASED PEROXISOMAL FATTY-ACID BETA-OXIDATION IN RATS FED [4-CHLORO-6-(2,3-XYLIDINO)-2-PYRIMIDINYLTHIO] ACETIC-ACID (WY-14,643) IN THE SEMIPURIFIED DIET [J].

LALWANI, ND ;

REDDY, MK ;

QURESHI, SA ;

REDDY, JK .

CARCINOGENESIS, 1981, 2 (07) :645-650

[8] INDUCTION POTENTIAL OF ANTIFUNGALS CONTAINING AN IMIDAZOLE OR TRIAZOLE MOIETY - MICONAZOLE AND KETOCONAZOLE, BUT NOT ITRACONAZOLE ARE ABLE TO INDUCE HEPATIC DRUG-METABOLIZING-ENZYMES OF MALE-RATS AT HIGH-DOSES [J].

LAVRIJSEN, K ;

VANHOUDT, J ;

THIJS, D ;

MEULDERMANS, W ;

HEYKANTS, J .

BIOCHEMICAL PHARMACOLOGY, 1986, 35 (11) :1867-1878

[9] KETOCONAZOLE BLOCKS ADRENAL STEROIDOGENESIS BY INHIBITING CYTOCHROME-P450-DEPENDENT ENZYMES [J].

LOOSE, DS ;

KAN, PB ;

HIRST, MA ;

MARCUS, RA ;

FELDMAN, D .

JOURNAL OF CLINICAL INVESTIGATION, 1983, 71 (05) :1495-1499

[10] INDUCTION OF CYTOSOLIC AND MICROSOMAL EPOXIDE HYDROLASES AND PROLIFERATION OF PEROXISOMES AND MITOCHONDRIA IN MOUSE-LIVER AFTER DIETARY EXPOSURE TO PARA-CHLOROPHENOXYACETIC ACID, 2,4-DICHLOROPHENOXYACETIC ACID AND 2,4,5-TRICHLOROPHENOXYACETIC ACID [J].

LUNDGREN, B ;

MEIJER, J ;

DEPIERRE, JW .

BIOCHEMICAL PHARMACOLOGY, 1987, 36 (06) :815-821

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