| Literature DB >> 15743710 |
Olga L Valenzuela1, Victor H Borja-Aburto, Gonzalo G Garcia-Vargas, Martha B Cruz-Gonzalez, Eliud A Garcia-Montalvo, Emma S Calderon-Aranda, Luz M Del Razo.
Abstract
Chronic exposure to inorganic arsenic (iAs) has been associated with increased risk of various forms of cancer and of noncancerous diseases. Metabolic conversions of iAs that yield highly toxic and genotoxic methylarsonite (MAsIII) and dimethylarsinite (DMAsIII) may play a significant role in determining the extent and character of toxic and cancer-promoting effects of iAs exposure. In this study we examined the relationship between urinary profiles of MAsIII and DMAsIII and skin lesion markers of iAs toxicity in individuals exposed to iAs in drinking water. The study subjects were recruited among the residents of an endemic region of central Mexico. Drinking-water reservoirs in this region are heavily contaminated with iAs. Previous studies carried out in the local populations have found an increased incidence of pathologies, primarily skin lesions, that are characteristic of arseniasis. The goal of this study was to investigate the urinary profiles for the trivalent and pentavalent As metabolites in both high- and low-iAs-exposed subjects. Notably, methylated trivalent arsenicals were detected in 98% of analyzed urine samples. On average, the major metabolite, DMAsIII, represented 49% of total urinary As, followed by DMAsV (23.7%), iAsV (8.6%), iAsIII (8.5%), MAsIII (7.4%), and MAsV (2.8%). More important, the average MAsIII concentration was significantly higher in the urine of exposed individuals with skin lesions compared with those who drank iAs-contaminated water but had no skin lesions. These data suggest that urinary levels of MAsIII, the most toxic species among identified metabolites of iAs, may serve as an indicator to identify individuals with increased susceptibility to toxic and cancer-promoting effects of arseniasis.Entities:
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Year: 2005 PMID: 15743710 PMCID: PMC1253747 DOI: 10.1289/ehp.7519
Source DB: PubMed Journal: Environ Health Perspect ISSN: 0091-6765 Impact factor: 9.031
Demographics of the study population.
| Low iAs exposure
| High iAs exposure
| ||||
|---|---|---|---|---|---|
| Characteristics | Control | Without skin lesions | With skin lesions | ||
| No. of subjects | 28 | 21 | 55 | ||
| Sex | |||||
| Male | 2 (7.1) | 1 (4.8) | 7 (14.6) | ||
| Female | 26 (92.9) | 20 (95.2) | 48 (85.4) | ||
| Age (years) | 35 (18–50) | 35 (21–49) | 35 (15–51) | ||
| Sunlight exposure (hours) | 2.3 (0–8) | 2.2 (0–8) | 2.8 (0–9) | ||
| TAs concentration in drinking water (μg/L) | 1.6 (1–6) | 117 (50–1,504) | 115 (50–658) | ||
| Duration of iAs exposure (years) | 26 (4–50) | 21 (4–49) | 26 (4–51) | ||
| TWE (mg) | 0.01 (0.01–0.06) | 5.8 (0.02–16.3) | 9.3 (0.23–26.9) | ||
Values are mean (range) except where noted.
Values are mean (%).
Duration of well water consumption.
Statistically significant difference (p < 0.05) between the exposed individuals with and without skin lesions.
Concentration and relative proportion of As species in residents of the Zimapan area (n = 104).
| iAs metabolite in urine | Concentration (μg/g creatinine) | Relative proportion (%) |
|---|---|---|
| iAsV | 5.84 (1–65.5) | 8.6 |
| iAsIII | 4.46 (0.1–172.3) | 8.5 |
| MAsV | 1.45 (0.1–28.3) | 2.8 |
| MAsIII | 4.93 (0.1–101.9) | 7.4 |
| DMAsV | 14.56 (1–710) | 23.7 |
| DMAsIII | 30.75 (0.1–506.3) | 49 |
| TAs | 84.85 (9.1–1398.1) | 100 |
Concentration of metabolites of As in urine are reported as geometric mean (range).
Distribution of skin lesion in iAs-exposed subjects (n = 76).
| Frequency [no. (%)]
| |||
|---|---|---|---|
| Skin lesion | With lesion | w/o lesion | |
| Hypopigmentation | 36 (47.4) | 40 (52.6) | |
| Hyperpigmentation | 29 (38.2) | 47 (61.8) | |
| Hypo-/hyperpigmentation | 9 (11.8) | 67 (88.2) | |
| Hyperkeratosis on the palms | 33 (43.4) | 43 (56.6) | |
| Hyperkeratosis on the soles | 30 (39.5) | 46 (60.5) | |
| Hyperkeratosis on the palms or soles | 43 (56.6) | 33 (43.4) | |
| Keratosis on the trunk | 17 (22.4) | 59 (77.6) | |
| Cutaneous horns | 4 (5.3) | 72 (94.7) | |
| Bowen’s disease | 1 (1.3) | 75 (98.7) | |
| Squamous cell carcinoma | 1 (1.3) | 75 (98.7) | |
w/o, without. Frequency was calculated for 76 subjects exposed to ≥ 50 μg/L As in drinking water.
Urinary pattern of iAs species in humans exposed to As through drinking water in the Zimapan area, according to level exposition and the presence of As skin lesions (n = 104).
| Metabolite concentration of iAs in urine (μg/g creatinine)
| ||||
|---|---|---|---|---|
| As species | Control ( | Exposed, without lesions ( | Exposed, with lesions ( | |
| IAsV | 3.6 (1.0–10.5) | 6.1 (2.0–37.2) | 8.2 (2.4–65.5) | |
| IAsIII | 1.6 (0.1–9.7) | 6.9 (1.5–101.6) | 6.3 (0.3–172.3) | |
| MAsV | 0.6 (0.1–5.5) | 1.8 (0.3–16.6) | 2.0 (0.1–28.3) | |
| MAsIII | 2.2 (0.4–9.6) | 4.8 (0.1–24.9) | 7.5 (0.2–101.9) | |
| DMAsV | 7.4 (1.8–38.5) | 15.9 (1.0–226.5) | 19.8 (1.0–710.1) | |
| DMAsIII | 7.9 (0.1–65.4) | 48.1 (2.2–206) | 51.9 (1.4–506.3) | |
| TAs | 33.3 (9.1–106) | 116 (61.2–371.7) | 121.2 (51.9–1,398) | |
Values shown are geometric mean (range).
Statistically significant difference (p < 0.05) between the exposed individuals with and without skin lesions (by Mann-Whitney test).
Comparison of mean percentage of As species in urine among As-exposed subjects with and without skin lesions.
| Percent As-exposed subjects
| |||
|---|---|---|---|
| As species | Without lesions ( | With lesions ( | |
| iAsV | 6.5 | 7.9 | |
| iAsIII | 10.9 | 8.0 | |
| MAsV | 3.5 | 2.3 | |
| MAsIII | 5.9 | 7.7 | |
| DMAsV | 21.5 | 23.1 | |
| DMAsIII | 51.7 | 51.0 | |
Statistically marginal difference (p = 0.072) between the exposed individuals with and without skin lesions (by Mann-Whitney test).