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5. Toxins in Botanical Drugs and Plant-derived Food and Feed – from Science to Regulation: A Workshop Review

Author

Schrenk, Dieter, Allemang, Ashley, Fahrer, Jörg, Harms, Henrik, Li, Xilin, Lin, Ge, Mahony, Catherine, Mulder, Patrick, Peijnenburg, Ad, Pfuhler, Stefan, Punt, Ans, Sievers, Hartwig, Troutman, John, Widjaja, Frances, Schrenk, Dieter, Allemang, Ashley, Fahrer, Jörg, Harms, Henrik, Li, Xilin, Lin, Ge, Mahony, Catherine, Mulder, Patrick, Peijnenburg, Ad, Pfuhler, Stefan, Punt, Ans, Sievers, Hartwig, Troutman, John, and Widjaja, Frances

Abstract

In September 2022, the 3rd International Workshop on pyrrolizidine alkaloids (PAs) and related phytotoxins was held on-line, entitled ʼToxins in botanical drugs and plant-derived food and feed – from science to regulationʼ. The workshop focused on new findings about the occurrence, exposure, toxicity, and risk assessment of PAs. In addition, new scientific results related to the risk assessment of alkenylbenzenes, a distinct class of herbal constituents, were presented. The presence of PAs and alkenylbenzenes in plant-derived food, feed, and herbal medicines has raised health concerns with respect to their acute and chronic toxicity but mainly related to the genotoxic and carcinogenic properties of several congeners. The compounds are natural constituents of a variety of plant families and species widely used in medicinal, food, and feed products. Their individual occurrence, levels, and toxic properties, together with the broad range of congeners present in nature, represent a striking challenge to modern toxicology. This review tries to provide an overview of the current knowledge on these compounds and indicates needs and perspectives for future research.

Published
2024

6. Dose addition in mixtures of compounds with dissimilar endocrine modes of action in in vitro receptor activation assays and the zebrafish sexual development test

Author

Bovee, Toine F.H., Heusinkveld, Harm J., Dodd, Sophie, Peijnenburg, Ad, Rijkers, Deborah, Blokland, Marco, Sprong, R.C., Crépet, Amélie, Nolles, Antsje, Zwart, Edwin P., Gremmer, Eric R., van der Ven, Leo T.M., Bovee, Toine F.H., Heusinkveld, Harm J., Dodd, Sophie, Peijnenburg, Ad, Rijkers, Deborah, Blokland, Marco, Sprong, R.C., Crépet, Amélie, Nolles, Antsje, Zwart, Edwin P., Gremmer, Eric R., and van der Ven, Leo T.M.

Abstract

Background: Human exposure to pesticides is being associated with feminisation for which a decrease of the anogenital distance (AGD) is a sensitive endpoint. Dose addition for the cumulative risk assessment of pesticides in food is considered sufficiently conservative for combinations of compounds with both similar and dissimilar modes of action (MoA). Objective: The present study was designed to test the dose addition hypothesis in a binary mixture of endocrine active compounds with a dissimilar mode of action for the endpoint feminisation. Methods: Compounds were selected from a list of chemicals of which exposure is related to a decrease of the AGD in rats and completed with reference compounds. These chemicals were characterised using specific in vitro transcriptional activation (TA) assays for estrogenic and androgenic properties, leading to a final selection of dienestrol as an ER-agonist and flutamide, linuron, and deltamethrin as AR-antagonists. These compounds were then tested in an in vivo model, i.e. in zebrafish (Danio rerio), using sex ratio in the population as an endpoint in order to confirm their feminising effect and MoA. Ultimately, the fish model was used to test a binary mixture of flutamide and dienestrol. Results: Statistical analysis of the binary mixture of flutamide and dienestrol in the fish sexual development tests (FSDT) with zebrafish supported dose addition.

Published
2024

9. Toxins in Botanical Drugs and Plant-derived Food and Feed – from Science to Regulation: A Workshop Review

Author

Schrenk, Dieter, additional, Allemang, Ashley, additional, Fahrer, Jörg, additional, Harms, Henrik, additional, Li, Xilin, additional, Lin, Ge, additional, Mahony, Catherine, additional, Mulder, Patrick, additional, Peijnenburg, Ad, additional, Pfuhler, Stefan, additional, Punt, Ans, additional, Sievers, Hartwig, additional, Troutman, John, additional, and Widjaja, Frances, additional

Published
2024
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16. New approach methodologies : A quantitative in vitro to in vivo extrapolation case study with PFASs

Author

Fragki, Styliani, Louisse, Jochem, Bokkers, Bas, Luijten, Mirjam, Peijnenburg, Ad, Rijkers, Deborah, Piersma, Aldert H., Zeilmaker, Marco J., Fragki, Styliani, Louisse, Jochem, Bokkers, Bas, Luijten, Mirjam, Peijnenburg, Ad, Rijkers, Deborah, Piersma, Aldert H., and Zeilmaker, Marco J.

Abstract

Per: and polyfluoroalkyl substances (PFASs) have been associated with increased blood lipids in humans. Perfluorooctanoic acid (PFOA) has been also linked with elevated alanine transferase (ALT) serum levels in humans, and in rodents the liver is a main target organ for many PFASs. With the focus on New Approach Methodologies, the chronic oral equivalent effect doses were calculated for PFOA, PFNA (perfluorononanoic acid), PFHxS (perfluorohexanesulfonic acid) and PFOS (perfluorooctane sulfonic acid) based on in vitro effects measured in the HepaRG cell line. Selected in vitro readouts were considered biomarkers for lipid disturbances and hepatotoxicity. Concentration-response data obtained from HepaRG cells on triglyceride (TG) accumulation and expression changes of 12 selected genes (some involved in cholesterol homeostasis) were converted into corresponding human dose-response data, using physiologically based kinetic (PBK) model-facilitated reverse dosimetry. Next to this, the biokinetics of the chemicals were studied in the cell system. The current European dietary PFASs exposure overlaps with the calculated oral equivalent effect doses, indicating that the latter may lead to interference with hepatic gene expression and lipid metabolism. These findings illustrate an in vitro-in silico methodology, which can be applied for more PFASs, to select those that should be prioritized for further hazard characterization.

Published
2023

17. Perfluoroalkyl substances (PFASs) decrease the expression of recombination-activating genes (RAG1 and RAG2) in human B lymphoma Namalwa cells

Author

Janssen, Aafke W.F., Louisse, Jochem, Rijkers, Deborah, Pinckaers, Nicole E.T., Hoekstra, Sjoerdtje A., Hoogenboom, Ron L.A.P., Peijnenburg, Ad A.C.M., Beekmann, Karsten, Janssen, Aafke W.F., Louisse, Jochem, Rijkers, Deborah, Pinckaers, Nicole E.T., Hoekstra, Sjoerdtje A., Hoogenboom, Ron L.A.P., Peijnenburg, Ad A.C.M., and Beekmann, Karsten

Abstract

Per- and polyfluoroalkyl substances (PFASs) are omnipresent and have been shown to induce a wide range of adverse effects, including hepatotoxicity, developmental toxicity and immunotoxicity. So far, little information is available about the mechanisms underlying the toxicity of PFASs, including those related to their immunotoxicity. Reported immunotoxic effects of PFASs include decreased antibody responses in experimental animals and humans, indicating that PFASs may, among others, affect B cell function. In the present study, we first assessed the effects of PFOA on the transcriptome of the human Namalwa B cell line using RNA seq analysis. Gene expression changes, analyzed using Ingenuity Pathway Analysis, pointed to various cellular processes affected by PFOA, including ‘B cell development’ and ‘Primary immunodeficiency signaling’. Interestingly, PFOA decreased the expression of RAG1 and RAG2, genes involved in immunoglobulin and T cell receptor V(D)J recombination. As a next step, time- and concentration-dependent changes in the expression of RAG1 and RAG2 upon exposure to PFOA, PFNA, PFHxS and PFOS were studied through RT-qPCR analysis. Analysis with the concentration–response modeling software PROAST resulted in the following potency ranking: PFNA > PFOA > PFOS > PFHxS. Altogether, the present in vitro study provides insights into the effects of selected PFASs on B cells, identifying RAG1 and RAG2 expression as possible relevant targets that may play a role in the immunotoxicity of PFASs.

Published
2023

27. Providing Biological Plausibility for Exposure–Health Relationships for the Mycotoxins Deoxynivalenol (DON) and Fumonisin B1 (FB1) in Humans Using the AOP Framework

Author

Van Den Brand, Annick D., Bajard, Lola, Steffensen, Inger-Lise, Brantsæter, Anne Lise, Dirven, Hubert A.A.M., Louisse, Jochem, Peijnenburg, Ad, Ndaw, Sophie, Mantovani, Alberto, De Santis, Barbara, Mengelers, Marcel J.B., Van Den Brand, Annick D., Bajard, Lola, Steffensen, Inger-Lise, Brantsæter, Anne Lise, Dirven, Hubert A.A.M., Louisse, Jochem, Peijnenburg, Ad, Ndaw, Sophie, Mantovani, Alberto, De Santis, Barbara, and Mengelers, Marcel J.B.

Abstract

Humans are chronically exposed to the mycotoxins deoxynivalenol (DON) and fumonisin B1 (FB1), as indicated by their widespread presence in foods and occasional exposure in the workplace. This exposure is confirmed by human biomonitoring (HBM) studies on (metabolites of) these mycotoxins in human matrices. We evaluated the exposure–health relationship of the mycotoxins in humans by reviewing the available literature. Since human studies did not allow the identification of unequivocal chronic health effects upon exposure to DON and FB1, the adverse outcome pathway (AOP) framework was used to structure additional mechanistic evidence from in vitro and animal studies on the identified adverse effects. In addition to a preliminary AOP for DON resulting in the adverse outcome (AO) ‘reduced body weight gain’, we developed a more elaborated AOP for FB1, from the molecular initiating event (MIE) ‘inhibition of ceramide synthases’ leading to the AO ‘neural tube defects’. The mechanistic evidence from AOPs can be used to support the limited evidence from human studies, to focus FB1- and DON-related research in humans to identify related early biomarkers of effect. In order to establish additional human exposure–health relationships in the future, recommendations are given to maximize the information that can be obtained from HBM. View Full-Text

Published
2022

31. Providing Biological Plausibility for Exposure–Health Relationships for the Mycotoxins Deoxynivalenol (DON) and Fumonisin B1 (FB1) in Humans Using the AOP Framework

Author

van den Brand, Annick D., primary, Bajard, Lola, additional, Steffensen, Inger-Lise, additional, Brantsæter, Anne Lise, additional, Dirven, Hubert A. A. M., additional, Louisse, Jochem, additional, Peijnenburg, Ad, additional, Ndaw, Sophie, additional, Mantovani, Alberto, additional, De Santis, Barbara, additional, and Mengelers, Marcel J. B., additional

Published
2022
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32. New approach methodologies (NAMs) for human-relevant biokinetics predictions

Author

Punt, Ans, Bouwmeester, Hans, Blaauboer, Bas J, Coecke, Sandra, Hakkert, Betty, Hendriks, Delilah F G, Jennings, Paul, Kramer, Nynke I, Neuhoff, Sibylle, Masereeuw, Rosalinde, Paini, Alicia, Peijnenburg, Ad A C M, Rooseboom, Martijn, Shuler, Michael L, Sorrell, Ian, Spee, Bart, Strikwold, Marije, Van der Meer, Andries D, Van der Zande, Meike, Vinken, Mathieu, Yang, Huan, Bos, Peter M J, Heringa, Minne B, Molecular and Computational Toxicology, AIMMS, Liver Connexin and Pannexin Research Group, Pharmaceutical and Pharmacological Sciences, Connexin Signalling Research Group, Experimental in vitro toxicology and dermato-cosmetology, and Applied Stem Cell Technologies

Subjects
in vitro, Animal Testing Alternatives, Toxicology, Risk Assessment, biokinetics, Hazardous Substances, SDG 17 - Partnerships for the Goals, BU Toxicologie, Novel Foods & Agroketens, in silico, next-generation risk evaluations, PB(P)K, Animals, Humans, BU Toxicology, Novel Foods & Agrochains, Toxicologie, VLAG, QIVIVE
Abstract

For almost fifteen years, the availability and regulatory acceptance of new approach methodologies (NAMs) to assess the absorption, distribution, metabolism and excretion (ADME/biokinetics) in chemical risk evaluations are a bottleneck. To enhance the field, a team of 24 experts from science, industry, and regulatory bodies, including new generation toxicologists, met at the Lorentz Centre in Leiden, The Netherlands. A range of possibilities for the use of NAMs for biokinetics in risk evaluations were formulated (for example to define species differences and human variation or to perform quantitative in vitro-in vivo extrapolations). To increase the regulatory use and acceptance of NAMs for biokinetics for these ADME considerations within risk evaluations, the development of test guidelines (protocols) and of overarching guidance documents is considered a critical step. To this end, a need for an expert group on biokinetics within the Organisation of Economic Cooperation and Development (OECD) to supervise this process was formulated. The workshop discussions revealed that method development is still required, particularly to adequately capture transporter mediated processes as well as to obtain cell models that reflect the physiology and kinetic characteristics of relevant organs. Developments in the fields of stem cells, organoids and organ-on-a-chip models provide promising tools to meet these research needs in the future.

Published
2020

35. Novel Insights into Pyrrolizidine Alkaloid Toxicity and Implications for Risk Assessment: Occurrence, Genotoxicity, Toxicokinetics, Risk Assessment–A Workshop Report

Author

Schrenk, Dieter, additional, Fahrer, Jörg, additional, Allemang, Ashley, additional, Fu, Peter, additional, Lin, Ge, additional, Mahony, Catherine, additional, Mulder, Patrick P.J., additional, Peijnenburg, Ad, additional, Pfuhler, Stefan, additional, Rietjens, Ivonne M.C.M., additional, Sachse, Benjamin, additional, Steinhoff, Barbara, additional, These, Anja, additional, Troutman, John, additional, and Wiesner, Jacqueline, additional

Published
2021
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37. Systemic PFOS and PFOA exposure and disturbed lipid homeostasis in humans : what do we know and what not?

Author

Fragki, Styliani S., Dirven, Hubert, Fletcher, Tony, Grasl-Kraupp, Bettina, Bjerve Gützkow, Kristine, Hoogenboom, Ron, Kersten, Sander, Lindeman, Birgitte, Louisse, Jochem, Peijnenburg, Ad, Piersma, Aldert H., Princen, Hans M.G., Uhl, Maria, Westerhout, Joost, Zeilmaker, Marco J., Luijten, Mirjam, Fragki, Styliani S., Dirven, Hubert, Fletcher, Tony, Grasl-Kraupp, Bettina, Bjerve Gützkow, Kristine, Hoogenboom, Ron, Kersten, Sander, Lindeman, Birgitte, Louisse, Jochem, Peijnenburg, Ad, Piersma, Aldert H., Princen, Hans M.G., Uhl, Maria, Westerhout, Joost, Zeilmaker, Marco J., and Luijten, Mirjam

Abstract

Associations between per- and polyfluoroalkyl substances (PFASs) and increased blood lipids have been repeatedly observed in humans, but a causal relation has been debated. Rodent studies show reverse effects, i.e. decreased blood cholesterol and triglycerides, occurring however at PFAS serum levels at least 100-fold higher than those in humans. This paper aims to present the main issues regarding the modulation of lipid homeostasis by the two most common PFASs, PFOS and PFOA, with emphasis on the underlying mechanisms relevant for humans. Overall, the apparent contrast between human and animal data may be an artifact of dose, with different molecular pathways coming into play upon exposure to PFASs at very low versus high levels. Altogether, the interpretation of existing rodent data on PFOS/PFOA-induced lipid perturbations with respect to the human situation is complex. From a mechanistic perspective, research on human liver cells shows that PFOS/PFOA activate the PPARα pathway, whereas studies on the involvement of other nuclear receptors, like PXR, are less conclusive. Other data indicate that suppression of the nuclear receptor HNF4α signaling pathway, as well as perturbations of bile acid metabolism and transport might be important cellular events that require further investigation. Future studies with human-relevant test systems would help to obtain more insight into the mechanistic pathways pertinent for humans. These studies shall be designed with a careful consideration of appropriate dosing and toxicokinetics, so as to enable biologically plausible quantitative extrapolations. Such research will increase the understanding of possible perturbed lipid homeostasis related to PFOS/ PFOA exposure and the potential implications for human health.

Published
2021

38. Correction: Cytochrome P450 expression, induction and activity in human induced pluripotent stem cell-derived intestinal organoids and comparison with primary human intestinal epithelial cells and Caco-2 cells

Author

Janssen, Aafke W.F., Duivenvoorde, Loes P.M., Rijkers, Deborah, Nijssen, Rosalie, Peijnenburg, Ad A.C.M., Zande, Meike, van der, Louisse, Jochem, Janssen, Aafke W.F., Duivenvoorde, Loes P.M., Rijkers, Deborah, Nijssen, Rosalie, Peijnenburg, Ad A.C.M., Zande, Meike, van der, and Louisse, Jochem

Abstract

In the original publication of the article, the dilution of DAPT in sentence “To promote intestinal differentiation,…” was published with an error. The “5 mM DAPT” should be “5 μM DAPT”. The original article has been updated with the correct dilution.

Published
2021

39. Development of a Web-Based Toolbox to Support Quantitative In-Vitro-to-In-Vivo Extrapolations (QIVIVE) within Nonanimal Testing Strategies

Author

Punt, Ans, Pinckaers, Nicole, Peijnenburg, Ad, Louisse, Jochem, Punt, Ans, Pinckaers, Nicole, Peijnenburg, Ad, and Louisse, Jochem

Abstract

The goal of the present study was to develop an online web-based toolbox that contains generic physiologically based kinetic (PBK) models for rats and humans, including underlying calculation tools to predict plasma protein binding and tissue:plasma distribution, to be used for quantitative in-vitro-to-in-vivo extrapolations (QIVIVE). The PBK models within the toolbox allow first estimations of internal plasma and tissue concentrations of chemicals to be made, based on the logP and pKa of the chemicals and values for intestinal uptake and intrinsic hepatic clearance. As a case study, the toolbox was used to predict oral equivalent doses of in vitro ToxCast bioactivity data for the food additives methylparaben, propyl gallate, octyl gallate, and dodecyl gallate. These oral equivalent doses were subsequently compared with human exposure estimates, as a low tier assessment allowing prioritization for further assessment. The results revealed that daily intake levels of especially propyl gallate can lead to internal plasma concentrations that are close to in vitro biological effect concentrations, particularly with respect to the inhibition of human thyroid peroxidase (TPO). Estrogenic effects were not considered likely to be induced by the food additives, as daily exposure levels of the different compounds remained 2 orders of magnitude below the oral equivalent doses for in vitro estrogen receptor activation. Overall, the results of the study show how the toolbox, which is freely accessible through www.qivivetools.wur.nl, can be used to obtain initial internal dose estimates of chemicals and to prioritize chemicals for further assessment, based on the comparison of oral equivalent doses of in vitro biological activity data with human exposure levels.

Published
2021

43. Deliverable D2.4 - Report on the integrated use of QSAR and TTC approaches to prioritise chemicals for further risk assessment in the context of mixtures

Author

Rorije, Emiel, Cotterill, Jane, Eberini, Ivano, and Peijnenburg, Ad

Abstract

This deliverable describes the overall workflow followed in EuroMix Work Package 2. This workflow, which is proposed to be used as a first tier in-silico risk assessment of chemical mixtures in general, consists of four steps: 1) The first step is the identification of chemicals in food or feed that are of interest for combined exposures. A list of 1598 substances has been identified specifically for the purpose of EuroMix, and is described in D2.1 “Report describing cumulative assessment groups for a broad range of chemicals, based on information extracted from (literature) databases” . This list – the EuroMix Chemical Inventory – is subsequently completed with the results from the in-silico tools and calculations performed in EuroMix Work Package 2, described in detail in Deliverables 2.2, 2.3 and this deliverable (see next steps). 2) Determining the probability that a chemical belongs to a certain Cumulative Assessment Group (CAG). The level at which CAGs need to be determined for mixture risk assessment (level 1, organ toxicity, level 2: organ effect phenotype, level 3: mode of action, i.e. cellular processes, and level 4: mechanism of action, or molecular initiating events) is not established yet, as indications for this should come from the experimental work packages in EuroMix. The present deliverable D2.4 outlines the work-flows using existing QSAR models described in EuroMix D2.2 (Report on the use of in‐silico methods for the prioritisation of substances and mixtures thereof), in combination with the results from detailed molecular docking calculations performed as new research in the EuroMix project and described in D2.3. 3) Assignment of a relative potency factor to each chemical that was considered in the previous step to be part of the CAG of interest. These relative potencies are used to scale the exposures of all mixture components. RPF derivation using Threshold of Toxicological Concern (TTC) concepts, and Molecular Docking results were described in D2.3. Additionally a proposal for the use of read across based on chemical similarity is given in this deliverable. Interpretation of molecular docking based RPFs, as well as the interpretation of in vitro modelling results from WP3 in EuroMix, requires In Vitro to In Vivo Extrapolation. A first (QSAR based) tier to IVIVE is presented in section 6 of this deliverable. 4) Finally the mixture risk is determined by adding up all the scaled exposures of the mixture components that are predicted to be part of the Cumulative Assessment Group. As exposure considerations are not taken into account at all at this stage – for a large part of the EuroMix Inventory no exposure data will be available – the final risk assessment calculations are not part of this Deliverable. This workflow and all the data obtained with the tools and model predictions will be implemented in the EuroMix software tool as part of the EuroMix Work Package 6. The individual tools used in the mixture risk assessment workflow can be used to do prioritizations and rankings, i.e. to find the (predicted) most potent substances for a specific CAG. In section 5 of this Deliverable, these prioritizations have been performed to generate lists of potentially interesting substances - based on their predicted effect / mechanism of action and potency – for further testing in the in-vitro toolbox (EuroMix work package 3).

Published
2020
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45. Additional file of An untargeted multi-technique metabolomics approach to studying intracellular metabolites of HepG2 cells exposed to 2,3,7,8-tetrachlorodibenzo-p-dioxin

Author

Ruiz-Aracama, Ainhoa, Peijnenburg, Ad, Kleinjans, Jos, Danyel Jennen, Delft, Joost Van, Hellfrisch, Caroline, and Lommen, Arjen

Abstract

Additional file of An untargeted multi-technique metabolomics approach to studying intracellular metabolites of HepG2 cells exposed to 2,3,7,8-tetrachlorodibenzo-p-dioxin

Published
2020
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