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Changes in the classification of carcinogenic chemicals in the work area (1998)

Neumann, H.-G. ; Thielmann, H. W. ; Filser, J. G. ; [et al.]

Springer

Journal of cancer research and clinical oncology 124 (1998), S. 661-669

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ISSN: 1432-1335

Keywords: Key words Chemical carcinogens ; List of MAK and BAT values ; Cancer risk ; carcinogen classification

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Carcinogenic chemicals in the work area were previously classified into three categories in section III of the German List of MAK and BAT values (the list of values on maximum workplace concentrations and bio‐logical tolerance for occupational exposures). This classification was based on qualitative criteria and reflected essentially the weight of evidence available for judging the carcinogenic potential of the chemicals. In the new classification scheme the former sections IIIA1, IIIA2, and IIIB are retained as categories 1, 2, and 3, to correspond with European Union regulations. On the basis of our advancing knowledge of reaction mechanisms and the potency of carcinogens, these three categories are supplemented with two additional categories. The essential feature of substances classified in the new categories is that exposure to these chemicals does not contribute significantly to the risk of cancer to man, provided that an appropriate exposure limit (MAK value) is observed. Chemicals known to act typically by non-genotoxic mechanisms, and for which information is available that allows evaluation of the effects of low-dose exposures, are classified in category 4. Genotoxic chemicals for which low carcinogenic potency can be expected on the basis of dose/response relationships and toxicokinetics and for which risk at low doses can be assessed are classified in category 5. The basis for a better differentiation of carcinogens is discussed, the new categories are defined, and possible criteria for classification are described. Examples for category 4 (1,4-dioxane) and category 5 (styrene) are presented.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s004320050229

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Recommendations for the categorization of germ cell mutagens (2000)

Adler, I.-D. ; Andrae, U. ; Kreis, P. ; [et al.]

Springer

International archives of occupational and environmental health 73 (2000), S. 428-432

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ISSN: 1432-1246

Keywords: Key words Germ cell mutagens ; List of MAK and BAT values ; Genetic risk

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Germ cell mutagens are currently classified into three categories in the German List of MAK and BAT Values. These categories have been revised and extended by analogy with the new categories for carcinogenic chemicals. Germ cell mutagens produce heritable gene mutations, and heritable structural and numerical chromosome aberrations in germ cells. The original categories 1 and 2 for germ cell mutagens remain unchanged. Two new categories 3A and 3B are proposed for chemicals suspected to be germ cell mutagens. A new category 5 is proposed for germ cell mutagens with low potency that contribute negligibly to human genetic risk provided the MAK value is observed.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s004200000122

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Biomonitoring of aromatic amines II: hemoglobin binding of some monocyclic aromatic amines (1988)

Birner, G. ; Neumann, H. -G.

Springer

Archives of toxicology 62 (1988), S. 110-115

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ISSN: 1432-0738

Keywords: Biological monitoring ; Hemoglobin binding ; Monocyclic aromatic amines ; Exposure control ; Risk assessment

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Covalent binding of 13 monocyclic aromatic amines to hemoglobin was studied in female Wistar rats and hemoglobin binding indices were determined. The hemoglobin adducts were hydrolyzed under alkaline conditions. In all cases the parent amine could be identified by gas chromatography and with one exception represented the only cleavage product. The binding index varied considerably and was highest withp-chloroaniline (569) and lowest with 2,4,5-trimethylaniline (0.7). Five compounds were also studied in female B6C3F1 mice. Hemoglobin binding was lower than in rats, but to varying degrees. Hemoglobin binding correlated remarkably well with the maximum methemoglobin level achieved with the six examples studied. The results support the notion that the reaction of nitrosoarenes, as metabolites of arylamines, with hemoglobin represents a general pathway in vivo. The analysis of such hemoglobin adducts is recommended as a dosimeter in biological monitoring of humans in order to control exposure. It is too early, however, to assess the carcinogenic risk from hemoglobin binding data with these compounds.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00570128

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Biomonitoring of aromatic amines III: Hemoglobin binding of benzidine and some benzidine congeners (1990)

Birner, G. ; Albrecht, W. ; Neumann, H. -G.

Springer

Archives of toxicology 64 (1990), S. 97-102

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ISSN: 1432-0738

Keywords: Biological monitoring ; Hemoglobin binding ; 4-Aminobiphenyl ; Benzidine ; 3,3′-Dichlorobenzidine ; 3,3′-Dimethoxybenzidine ; 3,3′-Dimethylbenzidine ; 3,3′,5,5′-Tetramethylbenzidine ; Direct red 28 ; Exposure control ; Risk assessment

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Covalent binding of benzidine and some congeners to hemoglobin was studied in female Wistar rats after oral administration. Hemoglobin adducts were hydrolyzed under alkaline conditions, and the arylamines extracted and analysed by HPLC with electrochemical detector. With benzidine, three cleavage products were observed, the major component being monoacetylbenzidine. This indicates that 4-nitroso-4′-N-acetylaminobiphenyl is the major reactive metabolite in erythrocytes. In addition benzidine and 4-aminobiphenyl were identified. The latter indicates a hitherto unknown metabolic pathway of benzidine. With 3,3′-dichlorobenzidine-dihydrochloride, 3,3′-dimethoxybenzidine and 3,3′-dimethylbenzidine two cleavage products were observed, the parent diamines being present in excess to or in amounts comparable to the monoacetyl derivative. With 3,3′,5,5′-tetramethylbenzidine a hemoglobin adduct could not be found. When the azo dye direct red 28 was administered to the animals, the three cleavage products typical for benzidine were found, indicating that benzidine became bioavailable after reductive cleavage of the azo compound. In this case the fraction of 4-aminobiphenyl was greater than after benzidine. It is proposed to use the analysis of hemoglobin adducts in human blood to control the exposure of individuals to these carcinogenic chemicals in the course of biochemical effect monitoring.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01974393

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