Literature DB >> 9255563

The role of human glutathione transferases and epoxide hydrolases in the metabolism of xenobiotics.

J Seidegård1, G Ekström.   

Abstract

Human glutathione transferases (GSTs) are a multigene family of enzymes that are involved in the metabolism of a wide range of electrophilic compounds of both exogenous and endogenous origin. GSTs are generally recognized as detoxifying enzymes by catalyzing the conjugation of these compounds with glutathione, but they may also be involved in activation of some carcinogens. The memmalian GSTs can be differentiated into four classes of cytosolic enzymes and two membrane bound enzymes. Human epoxide hydrolases (EHs) catalyze the addition of water to epoxides to form the corresponding dihydrodiol. The enzymatic hydration is essentially irreversible and produces mainly metabolites of lower reactivity that can be conjugated and excreted. The reaction of EHs is therefore generally regarded as detoxifying. The mammalian EHs can be distinguished by their physical and enzymatic properties. Microsomal EH (mEH) exhibits a broad substrate specificity, while the soluble EH (sEH) is an enzyme with a "complementary" substrate specificity to mEH. Cholesterol EH and leukotriene A4 hydrolase are two EHs with very limited substrate specificity. The activities of either GSTs or EHs expressed in vivo exhibit a relatively large interindividual variation, which might be explained by induction, inhibition, or genetic factors. These variations in levels or activities of individual isoenzymes are of importance with respect to an individual's susceptibility to genotoxic effects. This article gives a general overview of GSTs and EHs, discussing the modulation of activities, determination of these enzymes ex vivo, and the polymorphic expression of some isoenzymes.

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Year:  1997        PMID: 9255563      PMCID: PMC1470052          DOI: 10.1289/ehp.105-1470052

Source DB:  PubMed          Journal:  Environ Health Perspect        ISSN: 0091-6765            Impact factor:   9.031


  93 in total

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Authors:  B Mannervik
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Journal:  Hum Genet       Date:  1985       Impact factor: 4.132

4.  The distribution of microsomal glutathione transferase among different organelles, different organs, and different organisms.

Authors:  R Morgenstern; G Lundqvist; G Andersson; L Balk; J W DePierre
Journal:  Biochem Pharmacol       Date:  1984-11-15       Impact factor: 5.858

5.  Interindividual variations in the activities of cytosolic and microsomal epoxide hydrolase in human liver.

Authors:  I Mertes; R Fleischmann; H R Glatt; F Oesch
Journal:  Carcinogenesis       Date:  1985-02       Impact factor: 4.944

6.  Metabolism of xenobiotics in the human adrenal gland.

Authors:  D Papadopoulos; J Seidegard; J Rydström
Journal:  Cancer Lett       Date:  1984-02       Impact factor: 8.679

7.  The human glutathione S-transferases: studies on the tissue distribution and genetic variation of the GST1, GST2 and GST3 isozymes.

Authors:  R C Strange; C G Faulder; B A Davis; R Hume; J A Brown; W Cotton; D A Hopkinson
Journal:  Ann Hum Genet       Date:  1984-01       Impact factor: 1.670

8.  Existence of multiple forms of microsomal epoxide hydrolases with radically different substrate specificities.

Authors:  F Oesch; C W Timms; C H Walker; T M Guenthner; A Sparrow; T Watabe; C R Wolf
Journal:  Carcinogenesis       Date:  1984-01       Impact factor: 4.944

9.  Identification of a basic hybrid glutathione S-transferase from human liver. Glutathione S-transferase delta is composed of two distinct subunits (B1 and B2).

Authors:  P K Stockman; G J Beckett; J D Hayes
Journal:  Biochem J       Date:  1985-04-15       Impact factor: 3.857

10.  Measurement and characterization of membrane-bound and soluble epoxide hydrolase activities in resting mononuclear leukocytes from human blood.

Authors:  J Seidegård; J W DePierre; R W Pero
Journal:  Cancer Res       Date:  1984-09       Impact factor: 12.701

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  38 in total

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7.  Polymorphism in glutathione S-transferase P1 is associated with susceptibility to chemotherapy-induced leukemia.

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8.  Potent urea and carbamate inhibitors of soluble epoxide hydrolases.

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9.  The Independent and Combined Effects of Omega-3 and Vitamin B12 in Ameliorating Propionic Acid Induced Biochemical Features in Juvenile Rats as Rodent Model of Autism.

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10.  Elucidation of xenobiotic metabolism pathways in human skin and human skin models by proteomic profiling.

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