Literature DB >> 9223554

DMPS-arsenic challenge test. I: Increased urinary excretion of monomethylarsonic acid in humans given dimercaptopropane sulfonate.

H V Aposhian1, A Arroyo, M E Cebrian, L M del Razo, K M Hurlbut, R C Dart, D Gonzalez-Ramirez, H Kreppel, H Speisky, A Smith, M E Gonsebatt, P Ostrosky-Wegman, M M Aposhian.   

Abstract

The purpose of the present study was to evaluate in a novel manner the arsenic exposure of humans living in two towns in Northeastern Chile. Residents of one town drink water containing 593 microg As/l. Those in the control town drink water containing 21 microg As/l. Our hypothesis was that the administration of the chelating agent, 2,3-dimercaptopropane-1-sulfonic acid, Na salt (DMPS, DIMAVAL) would increase the urinary excretion of arsenic, alter the urinary profile of arsenic species and thus result in a better indication of the body load of arsenic and a better biomarker for arsenic exposure. The method used to evaluate these subjects was to give them 300 mg DMPS by mouth, after an overnight fast, and collect urine at specified time periods. The urine samples were analyzed for inorganic arsenic, monomethylarsonic acid (MMA), dimethylarsinic acid (DMA) and total arsenic by hydride generation and atomic absorption spectrophotometry. The results indicated that: 1) During the 2-hr period after DMPS administration, MMA represented 42%, inorganic As, 20 to 22% and DMA, 37 to 38% of the total urinary arsenic. The usual range of the MMA percentage in human urine has been 10 to 20%. The % MMA increased almost equally for both the arsenic-exposed and control subjects. 2) The exposed subjects had a greater urinary excretion of total arsenic, before and after DMPS administration, than the control subjects. 3) Although buccal cells were obtained only from a few subjects, the prevalence of mononucleated buccal cells, an indication of genotoxicity, was 5-fold greater for those who consumed drinking water with the higher arsenic content than among control subjects. Our conclusions are that 1) DMPS has a highly specific effect in humans on MMA metabolism and/or urinary excretion; 2) the human body stores substantial amounts of arsenic; and 3) the urinary arsenic concentration after DMPS administration may be more indicative of the body burden of arsenic because it was greater than that found before DMPS was given.

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Year:  1997        PMID: 9223554

Source DB:  PubMed          Journal:  J Pharmacol Exp Ther        ISSN: 0022-3565            Impact factor:   4.030


  12 in total

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3.  Genetic integrity of the human Y chromosome exposed to groundwater arsenic.

Authors:  Safdar Ali; Sher Ali
Journal:  BMC Med Genomics       Date:  2010-08-06       Impact factor: 3.063

Review 4.  Mercury toxicity and treatment: a review of the literature.

Authors:  Robin A Bernhoft
Journal:  J Environ Public Health       Date:  2011-12-22

5.  Arsenic: health effects, mechanisms of actions, and research issues.

Authors:  C O Abernathy; Y P Liu; D Longfellow; H V Aposhian; B Beck; B Fowler; R Goyer; R Menzer; T Rossman; C Thompson; M Waalkes
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6.  Arsenic-induced skin lesions among Atacameño people in Northern Chile despite good nutrition and centuries of exposure.

Authors:  A H Smith; A P Arroyo; D N Mazumder; M J Kosnett; A L Hernandez; M Beeris; M M Smith; L E Moore
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7.  Estimation of arsenic intake from drinking water and food (raw and cooked) in a rural village of northern Chile. Urine as a biomarker of recent exposure.

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8.  Urinary trivalent methylated arsenic species in a population chronically exposed to inorganic arsenic.

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9.  Profile of urinary arsenic metabolites during pregnancy.

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10.  Reduction in urinary arsenic levels in response to arsenic mitigation efforts in Araihazar, Bangladesh.

Authors:  Yu Chen; Alexander van Geen; Joseph H Graziano; Alexander Pfaff; Malgosia Madajewicz; Faruque Parvez; A Z M Iftekhar Hussain; Vesna Slavkovich; Tariqul Islam; Habibul Ahsan
Journal:  Environ Health Perspect       Date:  2007-02-05       Impact factor: 9.031

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