76 results on '"Beekmann K"'
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2. New approach methodologies to enhance human health risk assessment of immunotoxic properties of chemicals - a PARC (Partnership for the Assessment of Risk from Chemicals) project
3. Impact of lincosamides antibiotics on the composition of the rat gut microbiota and the metabolite profile of plasma and feces
4. Can the microbiome mediate the toxicity of environmental chemicals?
5. MCPD esters and glycidyl esters in food supplements of fish oils, algae oils, and krill oils
6. Deltas under pressure, guidelines to facilitate transition pathways
7. Deltas under pressure, guidelines tofacilitate transition pathways
8. Interindividual differences and similarities in in vitro human gut microbial degradation of fructoselysine and carboxymethyllysine
9. Strategies to evaluate in vitro in silico physiologically based kinetic (PBK) models as essential tool in next generation (animal-free) risk evaluations
10. Human biomonitoring to estimate exposure to deoxynivalenol and zearalenone: two human studies to support the establishment of urinary biomonitoring equivalents
11. Collection of human and environmental data on pesticide use in Europe and Argentina: Field study protocol for the SPRINT project
12. Influence of the gut microbiome on plasma metabolite patterns
13. Analysis of metabolome changes in the bile acid pool in feces and plasma of antibiotic-treated rats
14. Microbiome-related metabolite changes in gut tissue, cecum content and feces of rats treated with antibiotics
15. The influence of phase II conjugation on the biological activity of flavonoids
16. Si Powder Based Substrates and Wafer Equivalent Based Solar Cells: Results of the European Project ThinSi
17. Interference of flavonoids with enzymatic assays for the determination of free fatty acid and triglyceride levels
18. The influence of phase II conjugation on the biological activity of flavonoids
19. P24-06 Tackling interindividual differences in toxicokinetics of gut microbial metabolites by microbiome-competent PBK modeling.
20. Properties of posttreated low κ flowfill™ films and their stability after etch, resist and polymer strip processes
21. A selective CMP process for stacked low-k CVD oxide films
22. Integration of Flowfill and Forcefill for cost-effective via applications
23. Flowfill-Process as a New Concept for Inter-Metal-Dielectrics
24. Novel self-planarizing CVD oxide for interlayer dielectric applications.
25. Electrical and material stability of Orion™ CVD ultra low-k dielectric film for copper interconnection.
26. Properties of posttreated low k flowfill films and their stability after etch, resist and polymer strip processes
27. P19-58 Use of transcriptomic signatures of pesticide active substances in human kidney cells to support definition of cumulative assessment groups (CAGs) for risk assessment.
28. P15-07 Bridging the gap: uncovering the mechanisms of action underlying antibody reduction following PFAS exposure.
29. P01-55 The effect of in vitro distribution of polycyclic aromatic hydrocarbons (PAHs) on in vitro derived genotoxic potencies.
30. P01-28 The effects of chlorinated paraffins on thyroid hormone metabolism in human HepaRG cells.
31. OS01-03 Toward standardization of testing strategies for in vitro hepatic metabolism studies.
32. Transport of perfluoroalkyl substances across human induced pluripotent stem cell-derived intestinal epithelial cells in comparison with primary human intestinal epithelial cells and Caco-2 cells.
33. Physiologically based kinetic (PBK) modeling as a new approach methodology (NAM) for predicting systemic levels of gut microbial metabolites.
34. New approach methodologies to enhance human health risk assessment of immunotoxic properties of chemicals - a PARC (Partnership for the Assessment of Risk from Chemicals) project.
35. Determination of in vitro immunotoxic potencies of a series of perfluoralkylsubstances (PFASs) in human Namalwa B lymphocyte and human Jurkat T lymphocyte cells.
36. Physiologically-Based Pharmacokinetic Modeling of the Postbiotic Supplement Urolithin A Predicts its Bioavailability Is Orders of Magnitude Lower than Concentrations that Induce Toxicity, but also Neuroprotective Effects.
37. Differences in gut microbial fructoselysine degradation activity between breast-fed and formula-fed infants.
38. Perfluoroalkyl substances (PFASs) decrease the expression of recombination-activating genes (RAG1 and RAG2) in human B lymphoma Namalwa cells.
39. Inter- and Intraindividual Differences in the Capacity of the Human Intestinal Microbiome in Fecal Slurries to Metabolize Fructoselysine and Carboxymethyllysine.
40. Differences in kinetics and dynamics of endogenous versus exogenous advanced glycation end products (AGEs) and their precursors.
41. Predictive performance of next generation human physiologically based kinetic (PBK) models based on in vitro and in silico input data.
42. Collection of human and environmental data on pesticide use in Europe and Argentina: Field study protocol for the SPRINT project.
43. Species Differences in in vitro and Estimated in vivo Kinetics for Intestinal Microbiota Mediated Metabolism of Acetyl-deoxynivalenols.
44. An in vitro model for microbial fructoselysine degradation shows substantial interindividual differences in metabolic capacities of human fecal slurries.
45. Interindividual Differences in Human Intestinal Microbial Conversion of (-)-Epicatechin to Bioactive Phenolic Compounds.
46. An in vitro model to quantify interspecies differences in kinetics for intestinal microbial bioactivation and detoxification of zearalenone.
47. Antibiotic-Induced Changes in Microbiome-Related Metabolites and Bile Acids in Rat Plasma.
48. Use of Physiologically Based Kinetic Modeling to Predict Rat Gut Microbial Metabolism of the Isoflavone Daidzein to S-Equol and Its Consequences for ERα Activation.
49. Combining In Vitro Data and Physiologically Based Kinetic Modeling Facilitates Reverse Dosimetry to Define In Vivo Dose-Response Curves for Bixin- and Crocetin-Induced Activation of PPARγ in Humans.
50. Use of proteomics to detect sex-related differences in effects of toxicants: implications for using proteomics in toxicology.
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