Interest of genotyping and phenotyping of drug-metabolizing enzymes for the interpretation of biological monitoring of exposure to styrene

6533b7d4fe1ef96bd1261e80

RESEARCH PRODUCT

Interest of genotyping and phenotyping of drug-metabolizing enzymes for the interpretation of biological monitoring of exposure to styrene

Franz Oesch Michael Arand Beata Janasik Vincent Haufroid Sergio Ghittori Ari Hirvonen Nina Hangen Dominique Lison Jean-pierre Buchet Marek Jakubowski Enrico Bergamaschi Antonio Mutti Paola Manini D. Ligocka

subject

Adult Male Phenylglyoxylic acid Genotype Metabolite Urinary system Population 10050 Institute of Pharmacology and Toxicology 610 Medicine & health Urine Pharmacology Biology Polymerase Chain Reaction 3000 General Pharmacology Toxicology and Pharmaceutics Excretion chemistry.chemical_compound 1311 Genetics Genetics Humans Lymphocytes General Pharmacology Toxicology and Pharmaceutics education Genotyping Styrene Glutathione Transferase Epoxide Hydrolases education.field_of_study Polymorphism Genetic Glyoxylates Cytochrome P-450 CYP2E1 Environmental Exposure CYP2E1 Acetylcysteine Isoenzymes Phenotype Glutathione S-Transferase pi Biochemistry chemistry 570 Life sciences; biology Mandelic Acids Biomarkers Polymorphism Restriction Fragment Length Environmental Monitoring

description

In the field of occupational and/or environmental toxicology, the measurement of specific metabolites in urine may serve to assess exposure to the parent compounds (biological monitoring of exposure). Styrene is one of the chemicals for which biological monitoring programs have been validated and implemented in environmental and occupational medicine. However, inter-individual differences in the urinary excretion exist both for the main end-products (mandelic acid and phenylglyoxylic acid) and for its specific mercapturic acids (phenylhydroxyethylmercapturic acids, PHEMA). This limits to a certain extent the use of these metabolites for an accurate assessment of styrene exposure. In a group of 26 volunteers selected with relevant genotypes, and exposed to styrene vapours (50 mg/m3, 8 h) in an inhalation chamber, we evaluated whether genotyping or phenotyping relevant drug-metabolizing enzymes (CYP2E1, EPHX1, GSTM1, GSTT1 and GSTP1) may help to explain the observed inter-individual variability in the urinary metabolite excretion. Peripheral blood lymphocytes were used for genotyping and as reporter cells for the phenotyping of CYP2E1 and EPHX1. The GSTM1 genotype was clearly the most significant parameter explaining the variance in urinary PHEMA excretion (6-fold lower in GSTM1 null subjects; P0.0001) so that systematic GSTM1 genotyping should be recommended routinely for a correct interpretation of PHEMA urinary levels. Variant alleles CYP2E1*6 (7632TA) and His113EPHX1 were associated with a significant reduction of, respectively, the expression (P = 0.047) and activity (P = 0.022) of the enzyme in peripheral blood lymphocytes. In combination with GSTM1 genotyping, the phenotyping approach also contributed to improve the interpretation of urinary results, as illustrated by the combined effect of CYP2E1 expression and GSTM1 allelic status that explained 77% of the variance in PHEMA excretion and allows the recommendation of mercapturates as specific and reliable biomarkers of exposure to styrene.

year	journal	country	edition	language
2002-12-01

10.1097/00008571-200212000-00003 http://hdl.handle.net/2318/1623117