Literature DB >> 16339183

Using urinary biomarkers to elucidate dose-related patterns of human benzene metabolism.

Sungkyoon Kim1, Roel Vermeulen, Suramya Waidyanatha, Brent A Johnson, Qing Lan, Nathaniel Rothman, Martyn T Smith, Luoping Zhang, Guilan Li, Min Shen, Songnian Yin, Stephen M Rappaport.   

Abstract

Although the toxicity of benzene has been linked to its metabolism, the dose-related production of metabolites is not well understood in humans, particularly at low levels of exposure. We investigated unmetabolized benzene in urine (UBz) and all major urinary metabolites [phenol (PH), E,E-muconic acid (MA), hydroquinone (HQ) and catechol (CA)] as well as the minor metabolite, S-phenylmercapturic acid (SPMA), in 250 benzene-exposed workers and 139 control workers in Tianjin, China. Median levels of benzene exposure were approximately 1.2 p.p.m. for exposed workers (interquartile range: 0.53-3.34 p.p.m.) and 0.004 p.p.m. for control workers (interquartile range: 0.002-0.007 p.p.m.). (Exposures of control workers to benzene were predicted from levels of benzene in their urine.) Metabolite production was investigated among groups of 30 workers aggregated by their benzene exposures. We found that the urine concentration of each metabolite was consistently elevated when the group's median benzene exposure was at or above the following air concentrations: 0.2 p.p.m. for MA and SPMA, 0.5 p.p.m. for PH and HQ, and 2 p.p.m. for CA. Dose-related production of the four major metabolites and total metabolites (micromol/l/p.p.m. benzene) declined between 2.5 and 26-fold as group median benzene exposures increased between 0.027 and 15.4 p.p.m. Reductions in metabolite production were most pronounced for CA and PH<1 p.p.m., indicating that metabolism favored production of the toxic metabolites, HQ and MA, at low exposures.

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Year:  2005        PMID: 16339183     DOI: 10.1093/carcin/bgi297

Source DB:  PubMed          Journal:  Carcinogenesis        ISSN: 0143-3334            Impact factor:   4.944


  33 in total

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3.  The impact of saturable metabolism on exposure-response relations in 2 studies of benzene-induced leukemia.

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Review 4.  Low-dose metabolism of benzene in humans: science and obfuscation.

Authors:  Stephen M Rappaport; Sungkyoon Kim; Reuben Thomas; Brent A Johnson; Frederic Y Bois; Lawrence L Kupper
Journal:  Carcinogenesis       Date:  2012-12-07       Impact factor: 4.944

5.  Occupational exposure to formaldehyde, hematotoxicity, and leukemia-specific chromosome changes in cultured myeloid progenitor cells.

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Review 6.  Benzene exposure: an overview of monitoring methods and their findings.

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8.  Evidence that humans metabolize benzene via two pathways.

Authors:  Stephen M Rappaport; Sungkyoon Kim; Qing Lan; Roel Vermeulen; Suramya Waidyanatha; Luoping Zhang; Guilan Li; Songnian Yin; Richard B Hayes; Nathaniel Rothman; Martyn T Smith
Journal:  Environ Health Perspect       Date:  2009-02-19       Impact factor: 9.031

9.  Benzene exposure near the U.S. permissible limit is associated with sperm aneuploidy.

Authors:  Caihong Xing; Francesco Marchetti; Guilan Li; Rosana H Weldon; Elaine Kurtovich; Suzanne Young; Thomas E Schmid; Luoping Zhang; Stephen Rappaport; Suramya Waidyanatha; Andrew J Wyrobek; Brenda Eskenazi
Journal:  Environ Health Perspect       Date:  2010-01-06       Impact factor: 9.031

10.  Flexible meta-regression to assess the shape of the benzene-leukemia exposure-response curve.

Authors:  Jelle Vlaanderen; Lützen Portengen; Nathaniel Rothman; Qing Lan; Hans Kromhout; Roel Vermeulen
Journal:  Environ Health Perspect       Date:  2009-11-18       Impact factor: 9.031

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