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1

Electronic Resource

Experimental toxicology of formaldehyde (1987)

Bolt, H. M.

Springer

Journal of cancer research and clinical oncology 113 (1987), S. 305-309

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ISSN: 1432-1335

Keywords: Formaldehyde ; Mutagenicity ; Metabolism ; Biochemistry ; Carcinogenicity

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Formaldehyde is a reactive chemical which undergoes spontaneous reactions with various cellular constituents. Mutagenicity data may be interpreted on the background of this behavior. Mice are better able to reduce the irritating effect of formaldehyde than rats and to reduce their ventilation rate when formaldehyde acts on the respiratory tract. Subacute exposure of rats to concentrations higher than 2 ppm inhibits mucociliary clearance of the nasal epithelium and leads to progressive histological and ultrastructural lesions at this site. The occurrence of squamous cell carcinomas of the nasal epithelium of rats after 2 years inhalation of 14.3 ppm formaldehyde (CIIT study) is probably the result of chronic and recurrent local toxicity; this is supported by species differences in susceptibility to the tissue damaging and carcinogenic effect of formaldehyde (rat, mouse, hamster). Data on formaldehyde-DNA interaction further support the argument that a direct risk extrapolation from the formaldehyde effects in rats to those expected for man is not possible.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00397713

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2

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A comparative investigation of the metabolism of methyl bromide and methyl iodide in human erythrocytes (1990)

Hallier, E. ; Deutschmann, S. ; Reichel, C. ; [et al.]

Springer

International archives of occupational and environmental health 62 (1990), S. 221-225

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ISSN: 1432-1246

Keywords: Methyl chloride ; Methyl bromide ; Methyl iodide ; Human erythrocyte glutathione S-transferase ; Toxicity

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Human erythrocyte cytoplasm was incubated in head space vials with either methyl bromide or methyl iodide. The decline in concentration of the two methyl halides was monitored by gas chromatography. Simultaneously, the production of S-methylglutathione was determined by thin layer chromatography. In parallel experiments, boiled erythrocyte cytoplasm was used in order to determine non-enzymatic conjugation. Furthermore, inhibition experiments with sulfobromophthalein were performed. The results were compared with previous findings on the metabolism of methyl chloride. In contrast to methyl chloride, both methyl bromide and methyl iodide showed a significant non-enzymatic conjugation with glutathione. In addition, an enzymatic conjugation could be observed in the erythrocyte cytoplasm of the majority of the population, whereas a minority lacks this enzymatic activity. This is consistent with findings on methyl chloride. Inhibition experiments show that a minor form of the erythrocyte glutathione transferase may be responsible for the enzymatic conjugation. Of the three monchalogenated methanes, methyl bromide is the substrate with the highest affinity for the conjugating enzyme(s). In the case of methyl iodide, non-enzymatic reaction overweighs the enzymatic process. There are possible implications of the results for occupational health and the toxicity of the substances.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00379437

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3

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Pharmacokinetics of halogenated ethylenes in rats (1978)

Filser, J. G. ; Bolt, H. M.

Springer

Archives of toxicology 42 (1978), S. 123-136

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ISSN: 1432-0738

Keywords: Halogenated ethylenes ; Vinyl fluoride ; Vinylidene fluoride ; Vinyl chloride ; Vinylidene chloride ; Cis-dichloroethylene ; Trans-dichloroethylene ; Trichloroethylene ; Perchloroethylene ; Vinyl bromide ; Pharmacokinetics ; Metabolism

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Inhalation pharmacokinetics of the halogenated ethylenes vinyl fluoride (VF), vinylidene fluoride (VF2), vinyl chloride (VC1), vinylidene chloride (VC12), cis- and trans-dichloroethylene (cis-DCE and trans-DCE), trichloroethylene (Tri), perchloroethylene (Per), and vinyl bromide (VBr) have been comparatively studied in the rat. Rats were exposed in a closed inhalation system to various initial atmospheric levels of halogenated ethylenes, and the decline of atmospheric concentration was followed using gas Chromatographic analysis. From pharmacokinetic analysis of the experimental curves the following general patterns of the halogenated ethylenes were derived. Distribution of the compounds in the organism and in the gas phase is determined by physical factors. For practical purposes, a relation of the equilibrium constants with the volatilities of the compounds, expressed by the boiling points, may be used: compounds with a low boiling point are enriched in tissues much less than those of a higher boiling point, and vice versa. Compounds with high accumulation in tissues (Tri, Per) need much more time for completion of the equilibration process than more volatile compounds. Metabolic elimination of halogenated ethylenes is a saturable, dose-dependent process. If animals are exposed to atmospheric concentrations of a halogenated ethylene which exceed the “point of saturation (Sp)”, elimination is determined by a zero-order law, i.e., its rate is independent of the concentration of the compound. In contrast, below saturation normal first-order kinetics apply. If the rate of metabolic elimination is related to the concentrations of the compounds in the tissue compartment, very similar rates for first-order elimination of the different halogenated ethylenes are found. This suggests a common rate limiting factor applicable for the lower concentration range. The maximal velocities (V max) of metabolic elimination of halogenated ethylenes which are reached above the “saturation points” depend on the chemical structures of the individual compounds. In general, with the exception of Tri, further halogen substitution inhibits metabolic conversion. Of the halogenated ethylenes, VF2 and Per are extremely slowly metabolized. The present report also provides the data necessary for calculation of the rates of metabolism of halogenated ethylenes in rats at a given concentration of atmospheric exposure.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00316492

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4

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Inhalation pharmacokinetics based on gas uptake studies (1981)

Filser, J. G. ; Bolt, H. M.

Springer

Archives of toxicology 47 (1981), S. 279-292

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ISSN: 1432-0738

Keywords: Pharmacokinetics ; Metabolism ; Halogenated ethylenes ; Vinyl fluoride ; Vinylidene fluoride ; Vinyl chloride ; Vinylidene chloride ; cis-Dichloroethylene ; trans-Dichloroethylene ; Trichloroethylene ; Vinyl bromide

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract An improved pharmacokinetic model is described for inhalation of volatile xenobiotics from a closed gas phase system. This model is based on steady-state kinetics and covers metabolic elimination processes of either first-order, zero-order, or Michaelis-Menten characteristics. It is emphasized that the distribution of a volatile compound between gas phase and organism under steady-state conditions may be much different from a static equilibrium obtained in absence of metabolism, as it is observed after application of a metabolic inhibitor. A re-analysis of previous experimental data on dose-dependent pharmacokinetics of different haloethylenes reveals that, in general, the metabolic elimination processes of the rapidly equilibrating mono-haloethylenes (and vinylidene fluoride) can be resolved with excellent accuracy into sections of first-order and zero-order kinetics. Other compounds show a more smooth transition from first-order elimination (at lower atmospheric concentrations) into conditions of saturation (dichloroethylenes, trichloroethylene). The analyses are consistent with a recent concept of Andersen (1980) that metabolic elimination of inhaled xenobiotics is limited by either the capacity of metabolic enzymes or factors of transport to the metabolic sites.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00332394

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5

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DNA-binding assay of methyl chloride (1985)

Peter, H. ; Laib, R. J. ; Ottenwälder, H. ; [et al.]

Springer

Archives of toxicology 57 (1985), S. 84-87

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ISSN: 1432-0738

Keywords: Methyl chloride ; DNA ; Nucleoproteins

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Fischer-344 rats and B6C3F1 mice of both sexes were exposed in closed chambers to 14C-labeled methyl chloride. Different clearance values from the gas phase of the system indicated that, based on body weight, mice metabolized the test compound much faster than rats. After isolation of DNA and nucleoproteins from liver and kidneys radioactivity was found in all macromolecular samples; this was ascribed to metabolic C1-incorporation. Radioactivity incorporation was particularly high in DNA of mouse kidneys, suggesting a high turnover to active C1 bodies (formaldehyde, formate) in this tissue. Analyses of DNA samples from kidneys of female and male mice showed neither 7-N-methylguanine nor O6-methylguanine. Hence, the formation of tumors in B6C3F1 mice exposed to high concentrations of methyl chloride is not based on methylation of DNA in this tissue.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00343115

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6

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Species differences in butadiene metabolism between mice and rats evaluated by inhalation pharmacokinetics (1986)

Kreiling, R. ; Laib, R. J. ; Filser, J. G. ; [et al.]

Springer

Archives of toxicology 58 (1986), S. 235-238

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ISSN: 1432-0738

Keywords: 1,3-Butadiene ; Inhalation ; Pharmacokinetics ; Species differences ; Metabolism

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Metabolism of 1,3-butadiene to 1,2-epoxybutene-3 in rats follows saturation kinetics. Comparative investigation of inhalation pharmacokinetics in mice also revealed a saturation pattern. For both species “linear” pharmacokinetics apply at exposure concentrations below 1000 ppm 1,3-butadiene; saturation of butadiene metabolism is observed at atmospheric concentrations of about 2000 ppm. For mice metabolic clearance per kg body weight in the lower concentration range where first order metabolism applies was 7300ml×h−1 (rat: 4500 ml×h−1). Maximal metabolic elimination rate (Vmax) was 400 μmol×h−1 ×kg−1 (rat: 220 μmol ×h−1×kg−1). This shows that 1,3-butadiene is metabolized by mice at higher rates compared to rats. Based on these investigations, the metabolic elimination rates of butadiene in both species were calculated for the exposure concentrations applied in two inhalation bioassays with rats and with mice. The results show that the higher rate of butadiene metabolism in mice when compared to rats may only in part be responsible for the considerable difference in the susceptibility of both species to butadiene-induced carcinogenesis.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00297112

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7

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Formation and repair of DNA lesions in kidneys of male mice after acute exposure to methyl chloride (1990)

Ristau, C. ; Bolt, H. M. ; Vangala, R. R.

Springer

Archives of toxicology 64 (1990), S. 254-256

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ISSN: 1432-0738

Keywords: Alkaline elution ; DNA-protein cross-links ; DNA repair ; Methyl chloride ; Mouse kidney ; Single-strand breaks

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract The time-course of DNA lesions (DNA-protein cross-links, single-strand breaks) induced by high concentrations of methyl chloride (1000 ppm) was measured in renal tissue of male mice by means of the alkaline elution assay in order to gain an insight into repair processes. DNA-protein cross-links were removed at a fast rate, whereas single-strand breaks appeared to accumulate, even during repair of DNA-protein cross-links. However, 48 h after exposure to methyl chloride, neither of these lesions were detectable in mouse kidney. Both types of DNA damage were ascribed to the action of formaldehyde, an intermediate in methyl chloride metabolism which may react with nucleic acids and protein and interfere with DNA repair.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF02010734

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8

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Inhalation pharmacokinetics of 1,2-epoxybutene-3 reveal species differences between rats and mice sensitive to butadiene-induced carcinogenesis (1987)

Kreiling, R. ; Laib, R. J. ; Filser, J. G. ; [et al.]

Springer

Archives of toxicology 61 (1987), S. 7-11

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ISSN: 1432-0738

Keywords: Butadiene ; Epoxybutene ; Inhalation ; Species differences ; Metabolism ; Pharmacokinetics

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Comparative investigations of inhalation pharmacokinetics of 1,2-epoxybutene-3 (vinyl oxirane, the primary reactive intermediate of butadiene) revealed major differences in metabolism of this compound between rats and mice. Whereas in rats no indication of saturation kinetics of epoxybutene metabolism could be observed up to exposure concentrations of 5000 ppm, in mice saturation of epoxybutene metabolism becomes apparent at atmospheric concentrations of about 500 ppm. The estimated maximal metabolic rate (Vmax) in mice for epoxybutene was only 350 μmol×h−1×kg−1 (rats: 〉2600 μmol× h−1×kg−1). In the lower concentration range where first order metabolism applies (up to about 500 ppm) epoxybutene is metabolized by mice at higher rates compared to rats (metabolic clearance per kg body weight, mice: 24900 ml×h−1, rats: 13400 ml×h−1). Under these conditions the steady state concentration of epoxybutene in the mouse is about 10 times that in the rat. When mice are exposed to high concentrations of butadiene (〉2000 ppm; conditions of saturation of butadiene metabolism; closed exposure system) epoxybutene is exhaled by the animals, and its concentration in the gas phase increases with exposure time. At about 10 ppm epoxybutene signs of acute toxicity are observed. When rats are exposed to butadiene under similar conditions, the epoxybutene concentration reaches a plateau at about 4 ppm. Under these conditions hepatic non-protein sulfhydryl compounds are virtually depleted in mice but not in rats. We conclude that in addition to the higher rate of metabolism of butadiene in mice, limited detoxification and consequently accumulation of its primary reactive intermediate epoxybutene may be a major determinant for the higher susceptibility of mice to butadiene-induced carcinogenesis.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00324541

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9

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DNA adducts of halogenated hydrocarbons (1986)

Bolt, H. M. ; Laib, R. J. ; Peter, H. ; [et al.]

Springer

Journal of cancer research and clinical oncology 112 (1986), S. 92-96

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ISSN: 1432-1335

Keywords: Methyl chloride ; Methyl bromide ; 1,2-Dichloroethane ; 1,2-Dibromoethane ; Vinyl chloride ; Vinyl bromide ; Vinylidene chloride ; Trichloroethylene ; Perchloroethylene ; 2,2′-Dichloro-diethyl ether ; Acrylonitrile ; Vinyl acetate ; Vinyl carbamate

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Although formation of DNA adducts has been postulated for several halomethanes, no chemical identification of such adducts has been performed so far. There is, however, evidence that methyl chloride does not act biologically as a DNA methylating agent. 1,2-Dichloroethane and 1,2-dibromoethane are activated through conjugation with glutathione. There is some evidence for formation on an N-7 adduct of guanine which carries an ethyl-S-cysteinyl moiety. Extensive work has been published on adducts of vinyl chloride, both in vitro and in vivo. The major DNA adduct is 7-(2-oxoethyl)guanine; a minor adduct appears to be N2,3-ethenoguanine. Other “etheno” adducts, i.e., 1,N6-ethenoadenine and 3,N4-ethenocytosine, are readily formed with DNA, vinyl chloride, and a metabolizing system in vitro and with RNA in vivo, but are usually not detected as DNA adducts in vivo. The data on DNA alkylation by vinyl chloride (and vinyl bromide) metabolites are compared with those of structurally related compounds (acrylonitrile, vinyl acetate, vinyl carbamate).

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00404388

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