7 results on '"Yasmin Sommer"'
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2. Exposure to Substances by Use of Consumer Products
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Stefanie Klenow, Christiaan Delmaar, Friederike Neisel, Yasmin Sommer, Astrid Heiland, Thomas Rüdiger, Gerhard Heinemeyer, Annette Bitsch, Stefan Hahn, Ralph Pirow, Michal Wiecko, Annegret Blume, and Wolfgang Koch
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Personal hygiene ,business.industry ,Marketing ,Clothing ,business ,Tiered approach ,Hobby ,Exposure assessment - Abstract
This chapter focuses on consumer product-related exposure issues. It covers all non-food products that can release chemical substances and consumers may come into contact with. They include, for example, products used inside and around the home for personal hygiene, home maintenance, do it yourself, automotive care, hobby and craft, leisure, playing, home office, pet care, home pesticides, furniture, clothing, and yard and garden maintenance. They are regulated by a number of different regulations (see the following subchapters). Consumer exposures to these products may be direct or indirect. As pointed out in Sect. 3.2.7, they can be characterised by the release of the agent from the source, the transport from the source to the target person (pathway of exposure), and the kind of contact (route of exposure). The release is determined by the chemical’s concentration in an item (consumer product), its properties (e.g. volatility), how it is bonded in the matrix, and what stressors (e.g. temperature, and mechanical activity by the user) are present. These conditions of exposure can be described in general terms in the exposure scenario and by subsequent iterations in a tiered approach. This chapter gives an overview about exposure assessment with regard to consumer products, separated into mixtures and articles. It also focuses on specific issues of exposure assessment with respect to (European) chemicals and cosmetic regulation. Further, this chapter addresses particular issues for exposure estimation of nanoparticles and sprays and aerosols, as well as secondary exposures from house dust.
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- 2019
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3. Disinfection by-products in ballast water treatment: An evaluation of regulatory data
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Sangeeta Banerji, Barbara Werschkun, and Yasmin Sommer
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Pollution ,Ballast ,Environmental Engineering ,Ozone ,Halogenation ,Ultraviolet Rays ,media_common.quotation_subject ,Acetates ,Water Purification ,chemistry.chemical_compound ,Hazardous waste ,Waste Management and Disposal ,Nitrites ,Ships ,Water Science and Technology ,Civil and Structural Engineering ,media_common ,Brackish water ,Bromates ,Chemistry ,Ecological Modeling ,Hydrogen Peroxide ,Bromate ,Environmental chemistry ,Water treatment ,Bromoform ,Introduced Species ,Water Pollutants, Chemical ,Disinfectants ,Trihalomethanes - Abstract
To reduce the global spread of invasive aquatic species, international regulations will soon require reductions of the number of organisms in ballast water discharged by ships. For this purpose, ballast water treatment systems were developed and approved by an international procedure. These systems rely on established water treatment principles which, to different degrees, have been proven to generate disinfection by-products with hazardous properties but have only scarcely been investigated in marine environments. Our study evaluates the publicly available documentation about approved ballast water treatment systems with regard to by-product formation. The most commonly employed methods are chlorination, ozonation, and ultraviolet (UV) irradiation. Chlorination systems generate trihalomethanes, halogenated acetic acids, and bromate in substantially larger quantities than reported for other areas of application. Levels are highest in brackish water, and brominated species predominate, in particular bromoform and dibromoacetic acid. Ozonation, which is less frequently utilized, produces bromoform in lower concentrations but forms higher levels of bromate, both of which were effectively reduced by active carbon treatment. In systems based on UV radiation, medium pressure lamps are employed as well as UV-induced advanced oxidation. For all UV systems, by-product formation is reported only occasionally. The most notable observations were small increases in nitrite, hydrogen peroxide, halogenated methanes and acetic acids. The assessment of by-product formation during ballast water treatment is limited by the lacking completeness and quality of available information. This concerns the extent and statistical characterisation of chemical analysis as well as the documentation of the test water parameters.
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- 2012
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4. SULT1C3, an orphan sequence of the human genome, encodes an enzyme activating various promutagens
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Walter Meinl, Hansruedi Glatt, Yasmin Sommer, Heiko Schneider, and Claudia Donath
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Blotting, Western ,Toxicology ,Substrate Specificity ,law.invention ,Cytosol ,law ,Safrole ,Animals ,Humans ,Coding region ,Gene ,Chromatography, High Pressure Liquid ,chemistry.chemical_classification ,Expression vector ,Bacteria ,biology ,Genome, Human ,Mutagenicity Tests ,Nucleic acid sequence ,Intron ,General Medicine ,Molecular biology ,Enzyme assay ,Rats ,Enzyme ,chemistry ,Biochemistry ,biology.protein ,Recombinant DNA ,Spectrophotometry, Ultraviolet ,Sulfotransferases ,Mutagens ,Food Science - Abstract
The human genome contains a sequence that is homologous to genes encoding soluble sulphotransferases (SULTs) based on the nucleotide sequence and possible intron/exon splice sites. The putative coding sequence (termed SULT1C3) was synthesized and integrated into a bacterial expression vector. We used the cDNA-expressed protein for raising an antiserum and studying enzyme activities. No activity was detected with 4-nitrophenol and 1-naphthol, known substrates of all other members of the human SULT1 subfamily. The activity was also negligible with paracetamol, ethanol, 5-hydroxymethylfurfural, 2-hydroxymethylpyrene, 2-(alpha-hydroxy)ethylpyrene, and corticosterone, compounds for which we have developed sensitive enzyme assays with direct determination of the product by HPLC-UV, HPLC-fluorescence or HPLC-MS/MS. Since diverse sulpho conjugates are chemically reactive - often short-lived and mutagenic - we expressed SULT1C3 in Ames'Salmonella typhimurium strains TA1538 and TA100, as we had done with many other SULTs previously. The expression level of SULT1C3 protein amounted to 2% of the total cytosolic proteins, which is in the middle range of other SULTs expressed in this model. Using recombinant bacterial tester strains in mutagenicity assays, we observed SULT1C3-mediated activation of several large benzylic alcohols derived from alkylated polycyclic hydrocarbons: 1-hydroxymethylpyrene, both enantiomers of 1-(alpha-hydroxy)ethylpyrene, 6-hydroxymethylbenzo[a]pyrene and 6-hydroxymethylanthanthrene. 1'-Hydroxysafrole was the smallest molecule activated by SULT1C3 up to date. Our study demonstrates that SULT1C3 has sulphotransferase activity and that it prefers relatively large substrates. The substrates detected were activated to mutagens, which cannot be the regular function of the enzyme. The physiological substrates remain to be identified. Probably, they are relatively large, endogenous or common exogenous, molecules.
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- 2008
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5. Heterologous and transgenic models for studying genotoxic effects of contaminants produced by heat-treatment of food
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Walter Meinl, Hansruedi Glatt, Gisela Dobbernack, and Yasmin Sommer
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Biochemistry ,business.industry ,Transgene ,Heterologous ,General Medicine ,Biology ,Contamination ,Toxicology ,business ,Biotechnology - Published
- 2006
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6. Bioactivation of food genotoxicants 5-hydroxymethylfurfural and furfuryl alcohol by sulfotransferases from human, mouse and rat: a comparative study
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Walter Meinl, Bernhard H. Monien, Hansruedi Glatt, Albrecht Seidel, Benjamin Sachse, and Yasmin Sommer
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0301 basic medicine ,Sulfotransferase ,Health, Toxicology and Mutagenesis ,Food Contamination ,Toxicology ,Risk Assessment ,Catalysis ,Scavenger ,Adduct ,Furfuryl alcohol ,Activation, Metabolic ,03 medical and health sciences ,chemistry.chemical_compound ,Species Specificity ,Nucleophile ,Tandem Mass Spectrometry ,medicine ,Humans ,Furaldehyde ,Furans ,Carcinogen ,5-Hydroxymethylfurfural ,Food carcinogens ,General Medicine ,Arylsulfotransferase ,Adenosine ,Recombinant Proteins ,Isoenzymes ,Kinetics ,Metabolic pathway ,030104 developmental biology ,chemistry ,Biochemistry ,UPLC-MS/MS ,Carcinogens ,Chromatography, Liquid ,Toxicokinetics and Metabolism ,medicine.drug - Abstract
5-Hydroxymethylfurfural (HMF) and furfuryl alcohol (FFA) are moderately potent rodent carcinogens that are present in thermally processed foodstuffs. The carcinogenic effects were hypothesized to originate from sulfotransferase (SULT)-mediated bioactivation yielding DNA-reactive and mutagenic sulfate esters, a confirmed metabolic pathway of HMF and FFA in mice. It is known that orthologous SULT forms substantially differ in substrate specificity and tissue distribution. This could influence HMF- and FFA-induced carcinogenic effects. Here, we studied HMF and FFA sulfoconjugation by 30 individual SULT forms of humans, mice and rats. The catalytic efficiencies (kcat/KM) of HMF sulfoconjugation of human SULT1A1 (13.7 s−1 M−1), mouse Sult1a1 (15.8 s−1 M−1) and 1d1 (4.8 s−1 M−1) and rat Sult1a1 (5.3 s−1 M−1) were considerably higher than those of all other SULT forms investigated (≤0.73 s−1 M−1). FFA sulfoconjugation was monitored using adenosine as a nucleophilic scavenger for the reactive 2-sulfoxymethylfuran (t1/2 = 20 s at 37 °C). The resulting adduct N6-((furan-2-yl)methyl)-adenosine (N6-MF-A) was quantified by isotope-dilution UPLC-MS/MS. The rates of N6-MF-A formation showed that hSULT1A1 and its orthologues in mice and rats were also the most important contributors to FFA sulfoconjugation in each of the species. Taken together, the catalytic capacity of hSULT1A1 is comparable to that of mSult1a1 in mice, the species in which carcinogenic effects of HMF and FFA were detected. This is of primary concern due to the expression of hSULT1A1 in many different tissues. Electronic supplementary material The online version of this article (doi:10.1007/s00204-014-1392-6) contains supplementary material, which is available to authorized users.
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7. State of the art in human risk assessment of silver compounds in consumer products: a conference report on silver and nanosilver held at the BfR in 2012
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Matthias Noll, Ursula Banasiak, Alfonso Lampen, Mario E. Götz, Andreas Hensel, Astrid Epp, Gaby-Fleur Böl, Andreas Luch, Carsten Kneuer, Frank Herzberg, Bernd Schäfer, Jochen vom Brocke, Jutta Tentschert, Isabel Günther, and Yasmin Sommer
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Consumer Product Safety ,German Federal Institute for Risk Assessment (BfR) ,Silver ,Health, Toxicology and Mutagenesis ,Nanotechnology ,Toxicology ,Risk communication ,Meeting Reports ,Analytical methods ,media_common.cataloged_instance ,European union ,media_common ,Exposure assessment ,Risk assessment ,Low toxicity ,Silver resistance mechanisms ,General Medicine ,Environmental exposure ,Human exposure ,Assessment and regulation of nanomaterials ,Risk analysis (engineering) ,Environmental science ,Nanosilver ,Exposure data ,Consumer products - Abstract
In light of the broad spectrum of products containing nanosilver, the harmfulness of nanosilver to human health and the environment was intensively discussed at a conference held in February 2012 at the BfR. The conference agenda covered the aspects of analytics of nanosilver materials, human exposure and toxicology as well as effects on microorganisms and the environment. The discussion recovered major gaps related to commonly agreed guidelines for sample preparation and central analytical techniques. In particular, the characterization of the nanoparticles in complex matrices was regarded as a challenge which might become a pitfall for further innovation and application. Historical and anecdotal records of colloidal silver have been sometimes taken as empirical proof for the general low toxicity of nanosilver. Yet as reported herein, a growing number of animal studies following modern performance standards of toxicity testing have been carried out recently revealing well-characterized adverse effects on different routes of exposure in addition to argyria. Furthermore, recent approaches in exposure assessment were reported. However, consumer exposure scenarios are only starting to be developed and reliable exposure data are still rare. It was further widely agreed on the workshop that the use of silver may lead to the selection of silver resistant bacteria. With respect to its environmental behavior, it was suggested that nanosilver released to wastewater may have negligible ecotoxicological effects. Finally, the presentations and discussion on risk assessment and regulation of nanosilver applications gave insights into different approaches of risk assessment of nanomaterials to be performed under the various regulatory frameworks.
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