Relationship Between Glutathione Concentration and Metabolism of the Pyrrolizidine Alkaloid, Monocrotaline, in the Isolated, Perfused Liver

Relationship Between Glutathione Concentration and Metabolism of the Pyrrolizidine Alkaloid, Monocrotaline, in the Isolated, Perfused Liver

The influence of GSH concentration on metabolism of monocrotaline was examined in the isolated, perfused rat liver. Chloroethanol (0.37 mmol/kg), diethyl maleate (5.6 mmol/kg), and buthionine sulfoximine (72.9 mmol/kg) given in vivo reduced hepatic GSH from 3.7 μmol/g wet weight to 1.5, 0.6 and 0.9...

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Veröffentlicht in:Toxicology and applied pharmacology 1995, Vol.130 (1), p.132-139
Hauptverfasser: Yan, C.C., Huxtable, R.J.
Format: Artikel
Sprache:eng
Schlagworte:
ALCALOIDE
ALCALOIDES
ALKALOIDS
Analysis of Variance
Animals
Antimetabolites, Antineoplastic - toxicity
BILE
Bile - metabolism
BILIS
Biological and medical sciences
Buthionine Sulfoximine
CROTALARIA
CROTALARIA SPECTABILIS
DEHYDROMONOCROTALINE
DEPLETION
Ethylene Chlorohydrin - pharmacology
FOIE
GLUTATHION
GLUTATHIONE
Glutathione - analogs & derivatives
Glutathione - metabolism
GLUTATION
HIGADO
LIVER
Liver - drug effects
Liver - metabolism
Male
Maleates - pharmacology
Medical sciences
METABOLISM
METABOLISME
METABOLISMO
METABOLITE
METABOLITES
METABOLITOS
Methionine Sulfoximine - analogs & derivatives
Methionine Sulfoximine - pharmacology
Monocrotaline - administration & dosage
Monocrotaline - analogs & derivatives
Monocrotaline - metabolism
Monocrotaline - toxicity
PERFUSION
Plant poisons toxicology
PYRROLES
Pyrroles - metabolism
PYRROLIC METABOLITES
Pyrrolidonecarboxylic Acid
RAT
RATA
RATS
Rats, Sprague-Dawley
Thiazoles - pharmacology
Thiazolidines
Toxicology
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Zusammenfassung:The influence of GSH concentration on metabolism of monocrotaline was examined in the isolated, perfused rat liver. Chloroethanol (0.37 mmol/kg), diethyl maleate (5.6 mmol/kg), and buthionine sulfoximine (72.9 mmol/kg) given in vivo reduced hepatic GSH from 3.7 μmol/g wet weight to 1.5, 0.6 and 0.9 μmol/g, respectively. Livers were then perfused in vitro for 1 hr with monocrotaline (0.5 mM). GSH depletion had no effect on the total release of pyrrolic metabolites of monocrotaline. Depletion, however, markedly affected the pattern of pyrrole release. Biliary release of 7-glutathionyl-6,7-dihydro-1-hydroxymethyl-5 H-pyrrolizine (GSDHP) was reduced by up to 72%. Pretreatment with diethyl maleate or buthionine sulfoximine increased the level of protein-bound pyrroles in the liver by 107 and 84%, respectively. Such pyrroles are probably responsible for liver toxicity. GSH depletion also led to a doubling of dehydromonocrotaline release into the perfusate. This metabolite is probably responsible for the extrahepatic toxicity of monocrotaline. Release into perfusate of the relatively nontoxic metabolite, 6,7-dihydro-7-hydroxy-1-hydroxymethyl-5 H-pyrrolizine (DHP) was correspondingly decreased. Hepatic GSH content was increased to 4.4 μmol/g by pretreatment with oxo-4-thiazolidine carboxylate (4.76 mmol/kg). This agent increased total pyrrolic metabolites by 54%. Biliary release of GSDHP and perfusate release of dehydromonocrotaline and DHP were all increased. Thus, hepatic GSH levels regulate the metabolism of monocrotaline and dehydromonocrotaline and, consequently, the hepatic and extrahepatic toxicity of monocrotaline. GSH depletion leads to a switch from the biliary release of the mildly toxic GSDHP to the perfusate release of the highly toxic dehydromonocrotaline. GSH depletion also permits more dehydromonocrotaline in the liver to become available for macromolecular alkylation. These findings suggest that nutritional intake of sulfur-containing amino acids can influence the severity of pyrrolizidine poisoning.
ISSN:0041-008X
1096-0333
DOI:10.1006/taap.1995.1017