Literature DB >> 17062723

A physiological toxicokinetic model for inhaled propylene oxide in rat and human with special emphasis on the nose.

György A Csanády1, Johannes G Filser.   

Abstract

Chronic exposure to high concentrations of PO induced inflammation in the respiratory nasal mucosa (RNM) of rodents and, for concentrations >or= 300 ppm, caused nasal tumors. Considering the nose to be the most relevant target organ for PO-induced tumorigenicity, we developed a physiological toxicokinetic model for PO in rats and humans. It includes compartments for arterial, venous, and pulmonary blood, liver, muscle, fat, richly perfused tissues, lung, and nose. It simulates inhalation of PO, its distribution into tissues by blood flow, and its elimination by exhalation and metabolism. In nose, lung, and liver of rats, PO conjugation with glutathione (GSH), PO-induced GSH depletion, and formation of PO adducts to DNA are described. Also modeled are PO adducts to hemoglobin of rats and humans. Required partition coefficients and metabolic parameters were derived experimentally or from publications. In rats, simulated PO concentrations in blood and GSH levels in tissues agreed with measured data. If compared with reported values, levels of adducts with hemoglobin were underpredicted up to a factor of about 2. Adducts with DNA differed up to a factor of 3. Hemoglobin adducts predicted for PO-exposed workers were 1.5-1.9 times higher than the reported ones. Considering identical conditions of PO exposure, similar PO concentrations in RNM were modeled for rats and humans. Also, PO concentrations in blood, about 1/30th of those in RNM, were similar in both species. Since the model was evaluated on all available data in rats and humans, we consider it to be useful for estimating the risk from inhalation exposure to PO.

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Year:  2006        PMID: 17062723     DOI: 10.1093/toxsci/kfl140

Source DB:  PubMed          Journal:  Toxicol Sci        ISSN: 1096-0929            Impact factor:   4.849


  3 in total

1.  Kinetics of ethylene and ethylene oxide in subcellular fractions of lungs and livers of male B6C3F1 mice and male fischer 344 rats and of human livers.

Authors:  Qiang Li; György András Csanády; Winfried Kessler; Dominik Klein; Helmut Pankratz; Christian Pütz; Nadine Richter; Johannes Georg Filser
Journal:  Toxicol Sci       Date:  2011-07-23       Impact factor: 4.849

2.  Pharmacokinetic analysis of the chronic administration of the inert gases Xe and Ar using a physiological based model.

Authors:  Ira Katz; Jacqueline Murdock; Marc Palgen; Jan Pype; Georges Caillibotte
Journal:  Med Gas Res       Date:  2015-05-29

Review 3.  Sensory irritation as a basis for setting occupational exposure limits.

Authors:  Thomas Brüning; Rüdiger Bartsch; Hermann Maximillian Bolt; Herbert Desel; Hans Drexler; Ursula Gundert-Remy; Andrea Hartwig; Rudolf Jäckh; Edgar Leibold; Dirk Pallapies; Albert W Rettenmeier; Gerhard Schlüter; Gisela Stropp; Kirsten Sucker; Gerhard Triebig; Götz Westphal; Christoph van Thriel
Journal:  Arch Toxicol       Date:  2014-09-03       Impact factor: 5.153

  3 in total

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