Metabolism of triallate in Sprague-Dawley rats.  2.  Identification and quantitation of excreted metabolites

Nadeau, Ronn; Chott, Robert; Fujiwara, Hideji; Shieh, Huey‐Sheng; Logusch, Eugene W.

doi:10.1021/jf00025a029

Cited by 5 publications

(10 citation statements)

References 10 publications

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“…This mechanism was proposed for the TZD ring opening of troglitazone by Kassahun et al (2001). A similar mechanism was also proposed by Hackett et al (1993) and Nadeau et al (1993) for the metabolism of the herbicide, triallate. Direct oxidation of M22 to give M7, although possible, was not detected when M22 was incubated with NADPH-fortified liver microsomes.…”

Section: Discussionsupporting

confidence: 63%

IN VITRO METABOLISM OF MK-0767 [(±)-5-[(2,4-DIOXOTHIAZOLIDIN-5-YL)METHYL]-2-METHOXY-N-[[(4-TRIFLUOROMETHYL)-PHENYL] METHYL]BENZAMIDE], A PEROXISOME PROLIFERATOR-ACTIVATED RECEPTOR α/γ AGONIST. II. IDENTIFICATION OF METABOLITES BY LIQUID CHROMATOGRAPHY-TANDEM MASS SPECTROMETRY

Liu¹,

Karanam

Doss³

et al. 2004

Drug Metab Dispos

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The in vitro metabolism of MK-0767 [(؎)-5-[(2,4-dioxothiazolidin-5-yl) methyl]-2-methoxy-N-[[(4-trifluoromethyl)-phenyl] methyl]benzamide], a novel 2,4-thiazolidinedione (TZD)-containing peroxisome proliferator-activated receptor ␣/␥ agonist, was studied in rat, dog, monkey, and human liver microsomes and hepatocytes, as well as in recombinant human CYP3A4-containing microsomes. Twenty-two metabolites (some at trace levels) were detected by liquid chromatography-tandem mass spectrometry analysis. All appeared to be phase I metabolites except for a glucuronide conjugate of a hydroxylated metabolite that was detected at trace levels. A constant neutral loss scan experiment performed on a triple quadrupole mass spectrometer proved to be very useful for resolving the metabolites from endogenous compounds. It was observed that the initial site of metabolism of MK-0767 was at the TZD ring leading to two major metabolites, namely the 5-hydroxy-TZD metabolite (M24) and the mercapto metabolite (M22). The latter was formed via the cleavage of the TZD ring with the elimination of the carbonyl adjacent to the sulfur atom. The structure of M24 was established by accurate mass measurements and NMR analysis. This hydroxy-TZD metabolite might represent an important precursor for a group of metabolites formed by TZD ring opening and subsequent loss of the sulfur moiety. The mercapto metabolite, on the other hand, is probably the key precursor for the TZD ring-opened metabolites with retention of the sulfur, even though the detailed mechanism of the ring scission remains to be characterized. From these studies, it was concluded that the TZD ring was the major site of metabolism of MK-0767. All the metabolites produced in vitro from human preparations were detected in the corresponding preparations from the nonclinical species.

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Section: Discussionsupporting

confidence: 63%

IN VITRO METABOLISM OF MK-0767 [(±)-5-[(2,4-DIOXOTHIAZOLIDIN-5-YL)METHYL]-2-METHOXY-N-[[(4-TRIFLUOROMETHYL)-PHENYL] METHYL]BENZAMIDE], A PEROXISOME PROLIFERATOR-ACTIVATED RECEPTOR α/γ AGONIST. II. IDENTIFICATION OF METABOLITES BY LIQUID CHROMATOGRAPHY-TANDEM MASS SPECTROMETRY

Liu¹,

Karanam

Doss³

et al. 2004

Drug Metab Dispos

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“…Thiol 4 was formed early in the course of microsomal and S-9 incubations and was then consumed, most likely via oxidation to the sulfur acids 2 and 3. In vitro metabolite 4 displayed the same HPLC retention time relative to triallate as did an authentic standard (Nadeau et al, 1993). Thiol 4 was isolated from a quenched S-9 incubation mixture by extraction with ethyl acetate and was derivatized to a pentafluorobenzoic acid thioester using pentafluorobenzoyl chloride.…”

Section: Resultsmentioning

confidence: 98%

Metabolism of triallate in Sprague-Dawley rats. 3. In vitro metabolic pathways

Hackett¹,

Kotyk²,

Fujiwara³

et al. 1993

J. Agric. Food Chem.

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Rat liver enzyme preparations were used to investigate the mechanistic pathways of triallate metabolism. Incubation of [14C]triallate with NADPH-fortified microsomes gave rise to metabolites generated via a number of reaction types, including sulfur oxidation/hydrolysis and hydroxylation of the allylic thiol moiety accompanied by rearrangement. Addition of glutathione (GSH) to microsomal incubations resulted in the formation of GSH conjugates arising via conjugate addition of glutathione to metabolic intermediates such as trichloroacrolein. Addition of GSH to microsomal incubations inhibited the binding of triallate-derived radioactivity to microsomal proteins. Metabolite identification was accomplished by mass spectrometry and chemical synthesis and by a novel application of heteronuclear multiple quantum coherence (HMQC) NMR spectroscopy. Elucidation of the in vitro metabolism of triallate provides important mechanistic information regarding triallate metabolism in the laboratory rat.

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“…The a phase reflects elimination as well as absorption, distribution, and metabolism, and changes in these processes at the high-dose level would be reflected in a longer initial half-life of elimination. Differences in triallate metabolite distribution are also observed at the 5 and 500 mg/kg dose levels (Nadeau et al, 1993). The ß phase half-life is considerably longer than the a phase half-life for all groups (Table III).…”

Section: E B-mentioning

confidence: 85%

“…Unlabeled triallate used for dilution to the desired specific activity had a purity of 99%. Test materials were synthesized in the laboratories of Monsanto Agricultural Co., St. Louis, MO (Nadeau at al., 1993). Purchased chemicals were of reagent or scintillation grade.…”

Section: Methodsmentioning

confidence: 99%

“…The present paper describes the material balance, tissue distribution, and elimination kinetics in Sprague-Dawley rats orally dosed with isotopically labeled triallate. The following paper in this issue (Nadeau et al, 1993) describes the chemical identification of urinary and fecal metabolites excreted by these animals and outlines possible metabolic pathways accounting for metabolite formation. The final paper in this series (Hackett et al, 1993) describes an in vitro study of triallate metabolism using microsomal enzyme preparations obtained from Sprague-Dawley rats and provides a detailed mechanistic understanding of the formation and reactions of metabolic intermediates giving rise to observed in vivo rat metabolites.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Metabolism of triallate in Sprague-Dawley rats. 1. Material balance, tissue distribution, and elimination kinetics

Ridley¹,

Warren²,

Nadeau³

1993

J. Agric. Food Chem.

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Triallate isotopically labeled with 14C and 13C in the C-l allylic carbon position was administered orally to male and female Sprague-Dawley rats at dose levels of 5 and 500 mg/kg of body weight. Most of the dose was rapidly eliminated within 72 h after administration, and dose recoveries averaged 92% and 96 % for the low-dose and high-dose animals, respectively. Approximately 42-52 % of the dose was excreted via the urine and 33-46% via the feces. Expired 14C02 accounted for approximately 4% of the dose, while the residual carcass at sacrifice contained approximately 2%. Radioactivity in blood was associated principally with hemoglobin. Kinetics for whole-body elimination of radioactivity were consistent with a two-compartment open model. The half-life of the a phase varied from 5.9 to 22.8 h, and that of the ß phase from 171 to 265 h.

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Metabolism of triallate in Sprague-Dawley rats. 2. Identification and quantitation of excreted metabolites

Cited by 5 publications

References 10 publications

IN VITRO METABOLISM OF MK-0767 [(±)-5-[(2,4-DIOXOTHIAZOLIDIN-5-YL)METHYL]-2-METHOXY-N-[[(4-TRIFLUOROMETHYL)-PHENYL] METHYL]BENZAMIDE], A PEROXISOME PROLIFERATOR-ACTIVATED RECEPTOR α/γ AGONIST. II. IDENTIFICATION OF METABOLITES BY LIQUID CHROMATOGRAPHY-TANDEM MASS SPECTROMETRY

IN VITRO METABOLISM OF MK-0767 [(±)-5-[(2,4-DIOXOTHIAZOLIDIN-5-YL)METHYL]-2-METHOXY-N-[[(4-TRIFLUOROMETHYL)-PHENYL] METHYL]BENZAMIDE], A PEROXISOME PROLIFERATOR-ACTIVATED RECEPTOR α/γ AGONIST. II. IDENTIFICATION OF METABOLITES BY LIQUID CHROMATOGRAPHY-TANDEM MASS SPECTROMETRY

Metabolism of triallate in Sprague-Dawley rats. 3. In vitro metabolic pathways

Metabolism of triallate in Sprague-Dawley rats. 1. Material balance, tissue distribution, and elimination kinetics

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