Publications by authors named "Leonie S Lautz"

The open source database "OpenCYP database" has been developed based on the results of extensive literature searches from the peer-reviewed literature. OpenCYP provides data on human variability on baseline of activities and polymophism frequencies for selected cytochrome P-450 isoforms (CYP1A2, CYP2A6, CYP2D6, CYP3A4/3A5 and CYP3A7) in healthy adult populations from world populations. CYP enzymatic activities were generally expressed as the metabolic ratio (MR) between an unchanged probe drug and its metabolite(s) in urine or plasma measured in healthy adults.

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Physiologically-based kinetic (PBK) models can simulate concentrations of chemicals in tissues over time without animal experiments. Nevertheless, in vivo data are often used to parameterise PBK models. This study aims to illustrate that a combination of kinetic and dynamic readouts from in vitro assays can be used to parameterise PBK models simulating neurologically-active concentrations of xenobiotics.

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Article Synopsis
  • Chemical pollution harms water quality and the natural benefits (called ecosystem services) we get from water systems.
  • The study created a new method to measure how pollution affects these services by looking at how many species might be harmed.
  • The results showed that pollution leads to a loss of these valuable services, and the study offers a way for water managers to make better choices to fix pollution problems.
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Article Synopsis
  • * It presents new findings on the variability of GST activities in healthy humans, highlighting the high inter-individual differences, tissue localization, and genetic polymorphisms of GSTs based on a comprehensive literature review and meta-analysis.
  • * The study emphasizes the importance of GSTs in responding to chemical stressors and calls for more research to identify specific substrates and quantitatively assess individual variations in GST activity, as current data is limited and often uncertain.
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In chemical risk assessment, default uncertainty factors are used to account for interspecies and interindividual differences, and differences in toxicokinetics and toxicodynamics herein. However, these default factors come with little scientific support. Therefore, our aim was to develop an in vitro method, using acetylcholinesterase (AChE) inhibition as a proof of principle, to assess both interspecies and interindividual differences in toxicodynamics.

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