Mathematical model insights into arsenic detoxification

Mathematical model insights into arsenic detoxification

Arsenic in drinking water, a major health hazard to millions of people in South and East Asia and in other parts of the world, is ingested primarily as trivalent inorganic arsenic (iAs), which then undergoes hepatic methylation to methylarsonic acid (MMAs) and a second methylation to dimethylarsinic...

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Veröffentlicht in:Theoretical biology and medical modelling 2011-08, Vol.8 (1), p.31-31, Article 31
Hauptverfasser: Lawley, Sean D, Cinderella, Molly, Hall, Megan N, Gamble, Mary V, Nijhout, H Frederik, Reed, Michael C
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Arsenic - pharmacokinetics
Arsenic - toxicity
Arsenic - urine
Arsenic compounds
Bangladesh
Demographic aspects
Dietary Supplements
Enzyme kinetics
Epidemiology
Experiments
Folic Acid - pharmacology
Health aspects
Health sciences
Heavy metals
Hepatocytes - drug effects
Hepatocytes - metabolism
Homocysteine
Human subjects
Humans
Inactivation, Metabolic
Kinetics
Liver diseases
Mathematical models
Metabolism
Metabolites
Methylation - drug effects
Models, Biological
Public health
Rats
Risk factors
Vitamin B
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Zusammenfassung:Arsenic in drinking water, a major health hazard to millions of people in South and East Asia and in other parts of the world, is ingested primarily as trivalent inorganic arsenic (iAs), which then undergoes hepatic methylation to methylarsonic acid (MMAs) and a second methylation to dimethylarsinic acid (DMAs). Although MMAs and DMAs are also known to be toxic, DMAs is more easily excreted in the urine and therefore methylation has generally been considered a detoxification pathway. A collaborative modeling project between epidemiologists, biologists, and mathematicians has the purpose of explaining existing data on methylation in human studies in Bangladesh and also testing, by mathematical modeling, effects of nutritional supplements that could increase As methylation. We develop a whole body mathematical model of arsenic metabolism including arsenic absorption, storage, methylation, and excretion. The parameters for arsenic methylation in the liver were taken from the biochemical literature. The transport parameters between compartments are largely unknown, so we adjust them so that the model accurately predicts the urine excretion rates of time for the iAs, MMAs, and DMAs in single dose experiments on human subjects. We test the model by showing that, with no changes in parameters, it predicts accurately the time courses of urinary excretion in mutiple dose experiments conducted on human subjects. Our main purpose is to use the model to study and interpret the data on the effects of folate supplementation on arsenic methylation and excretion in clinical trials in Bangladesh. Folate supplementation of folate-deficient individuals resulted in a 14% decrease in arsenicals in the blood. This is confirmed by the model and the model predicts that arsenicals in the liver will decrease by 19% and arsenicals in other body stores by 26% in these same individuals. In addition, the model predicts that arsenic methyltransferase has been upregulated by a factor of two in this population. Finally, we also show that a modification of the model gives excellent fits to the data on arsenic metabolism in human cultured hepatocytes. The analysis of the Bangladesh data using the model suggests that folate supplementation may be more effective at reducing whole body arsenic than previously expected. There is almost no data on the upregulation of arsenic methyltransferase in populations chronically exposed to arsenic. Our model predicts upregulation by a factor of two in the
ISSN:1742-4682
1742-4682
DOI:10.1186/1742-4682-8-31