4,868 results on '"toxicologie"'
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2. SĂNĂTATEA OCUPAȚIONALĂ, SIGURANȚĂ CHIMICĂ ȘI TOXICOLOGIE: PROTECȚIA SĂNĂTĂȚII – PENTRU UN VIITOR SIGUR
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Nicolae Jelamschi, Vasile Guștiuc, Ion Bahnarel, Grigore Friptuleac, Kristina Stîncă, Svetlana Gherciu-Tutuescu, Elena Bucata, Raisa Deleu, and Iurie Pînzaru
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sănătate ocupațională ,siguranță chimică ,toxicologie ,sănătate publică ,impact ,Medicine ,Surgery ,RD1-811 - Abstract
Scopul prezentei lucrări constă în identificarea poziției actuale ale sănătății ocupaționale, siguranței chimice și toxicologiei, în contextul actual al dezvoltării Republicii Moldova, și trasarea obiectivelor pe durata medie și lungă. S-a efectuat o analiză retrospectivă a realizărilor cercetării și practicii sănătății ocupaționale, siguranței chimice și toxicologiei în Republica Moldova. În calitate de material primar au servit referințele bibliografice cu tematica respectivă, datele bazelor de date cu acces deschis, atât naționale cât și internaționale. Au fost punctate direcțiile strategice de activitate în domeniul sănătății ocupaționale, siguranței chimice și toxicologiei. Dezvoltarea rețelei naționale a locurilor de muncă care promovează sănătatea, cu implementarea bunelor practici internaționale este un imperativ al timpului.
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- 2022
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3. Drug eruptions in children: About 121 cases.
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Hali, F., El Arabi, Y., El Fetoiki, F.Z., Kaddioui, Z., Marnissi, F., Dahbi Skali, H., Filali, H., and Chiheb, S.
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- 2022
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4. [Exavir: Implementation and evaluation of experimental pharmacology skills acquisition by pharmacy students].
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Bourreau C, Chevrier T, Desserrey T, Lusson N, Bessaguet F, Faure S, and Legeay S
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- Humans, Pilot Projects, Animals, Animal Experimentation, Software, France, Students, Pharmacy, Education, Pharmacy, Pharmacology education, Curriculum
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With the evolution of European and French regulations on animal experimentation in higher education, taking greater account of animal welfare, the University of Angers has developed a virtual animal experimentation software named Exavir. Used for practical work (PW) in physiology, pharmacology and toxicology in the Health, Sciences, and engineering curricula, Exavir can be used to simulate various experiments for teaching purposes, in vivo or ex vivo. Thanks to an original approach integrating serious games with different scenarios, students gain autonomy and become directly involved in their learning. In addition, Exavir's collaborative and participative development approach fosters inter-university partnerships and the emergence of innovative teaching methods. A hybrid pilot study carried out on a sample of 22 students in the Pharmacy Department of the Faculty of Health showed that Exavir improved students' acquisition of teaching skills in both physiology and pharmacology, compared with practical work only based on animal organs. These encouraging results demonstrate for the first time the pedagogical advantages of Exavir and confirm the interest in developing such a platform. In this context, it appears that Exavir also opens up the possibility of adapting the practical work offered within universities, and thus responding to the changing ethical issues of the coming decades., (Copyright © 2024 Académie Nationale de Pharmacie. Published by Elsevier Masson SAS. All rights reserved.)
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- 2024
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5. Actualités toxicologiques sur la 3,4-méthylènedioxymétamphétamine.
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Labat, Laurence, Boukerma, Khaled, and Houzé, Pascal
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La 3,4-méthylènedioxymétamphétamine (MDMA) ou ecstasy est connue comme drogue récréative illégale et connaît actuellement un regain d'intérêt dans les soirées festives auprès des jeunes. Elle est consommée pour ses effets empathogènes et entactogènes et les nouvelles tendances de consommations dans ce type de soirées l'associent fréquemment au GHB et à l'alcool. Des comprimés très colorés et de formes variées sont retrouvés sur les marchés pour être les plus attractifs possible. Et ces dernières années, on observe une nette augmentation de leurs teneurs en MDMA. Le dépistage rapide de la MDMA par méthodes immunochimiques peut être réalisé sur des automates de laboratoire ou sur des tests rapides sur les urines ou plus récemment sur des prélèvements salivaires. Une méthode de confirmation en chromatographie couplée à de la spectrométrie de masse permet d'identifier de façon spécifique la MDMA parmi les différentes et nombreuses structures amphétaminiques. Ces recherches et/ou dosages peuvent être réalisées sur de nombreuses matrices biologiques (sang, urine, salive, cheveux etc.) dans des contextes cliniques ou en médico-légal. Les tableaux d'intoxications fatales ou non fatales avec atteinte hépatique sont rapportés dans la littérature avec des concentrations très variables observées. 3,4-methylenedioxymetamphetamine (MDMA) or ecstasy is known as an illegal recreational drug and is currently experiencing renewed interest in festive evenings with young people. It is consumed for its empathetic and entactogenic effects and new consumption trends in this type of evening frequently associate it with GHB and alcohol. Very colorful tablets of various shapes are found on the markets to be the most attractive possible. And in recent years, there has been a marked increase in their MDMA content. Rapid testing of MDMA by immunochemical methods can be performed on laboratory automata or on urine rapid tests or more recently on salivary samples. À confirmation method in chromatography coupled with mass spectrometry makes it possible to identify specifically MDMA among the different amphetamine structures. This research and/or assays can be performed on many biological matrices (blood, urine, saliva, hair, etc.) in clinical or forensic cases. Fatal or non-fatal poisoning with hepatic involvement are reported in literature with variability in concentrations described. [ABSTRACT FROM AUTHOR]
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- 2021
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6. Les différents usages du cannabis : approche adaptée du biologiste toxicologue.
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Thiebot, Pauline and Labat, Laurence
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Le cannabis désigne le plus souvent la drogue récréative extraite de la plante Cannabis sativa. Son principal composé actif connu est le ∆-9-tétrahydrocannabinol (∆9-THC), responsable des effets psychotropes recherchés lors de sa consommation. Bien que prohibé et classé au registre des substances stupéfiantes dans la plupart des pays, le cannabis reste la drogue la plus consommée au monde à ce jour, avec près de 200 millions de consommateurs, loin devant les opioïdes et les amphétamines. Depuis les années 2010, l'utilisation de cannabinoïdes de synthèse, appartenant aux nouvelles substances psychoactives (NPS), est plus courante. Ces analogues chimiques du ∆9-THC présentent les mêmes effets que ce dernier, mais avec plus de puissance. Le second cannabinoïde le plus connu est le cannabidiol, ou CBD, aussi retrouvé dans la plante de Cannabis sativa. Il est sans activité psychotrope, et utilisé dans un but souvent anxiolytique. Plusieurs propriétés thérapeutiques sont revendiquées à ces molécules dans le domaine médical. Ainsi, de nombreux pays ont légalisé le commerce et l'utilisation des cannabinoïdes en tant que complément alimentaire ou en tant que médicament. L'analyse toxicologique permettra de distinguer les profils de consommation (intoxication ou surveillance de traitement...). Un dépistage urinaire immunologique permettra la détection d'une consommation de cannabis récréatif, tandis que la chromatographie couplée à la spectrométrie de masse permettra via un screening de surveiller l'apparition d'une nouvelle molécule cannabinoïde (NPS), ou bien permettra d'assurer un suivi thérapeutique d'un patient sous traitement cannabinoïde par un dosage spécifique des différentes molécules et de leurs métabolites. Cannabis commonly refers to the recreational drug extracted from the Cannabis sativa plant. Its main known active coumpound is ∆-9-tetrahydrocannabinol (∆9-THC), responsible for the psychotropic effects sought during its consumption. Though it is prohibited and classified in the register of narcotic substances in most countries, cannabis remains the most widely used drug in the world to date, with nearly 200 million users, far ahead opioids and amphetamines. Since the 2010s, the use of synthetic cannabinoids, which belong to the New Psychoactive Substances (NPS), is more frequent. These chemical analogues of ∆9-THC exhibit the same effects as the latter, but with more potency. The second best-known cannabinoid is cannabidiol, or CBD, also extracted from Cannabis sativa. It has no psychotropic activity and is often used as an anxiolytic. Several therapeutic properties are claimed for these molecules in the medical field. Thus, several countries have legalized trade and use of cannabinoids, as a dietary supplement or as a medicine. Toxicological analysis will make it possible to distinguish consumption profiles (intoxication or treatment monitoring, etc.). Immunological urinary screening will allow detection of recreational cannabis consumption while chromatography coupled with mass spectrometry will allow, thanks to a screening, monitoring the appearance of a new cannabinoid molecule (NPS), or will ensure therapeutic monitoring of a patient under cannabinoid treatment by a specific dosage of the various molecules and their metabolites. [ABSTRACT FROM AUTHOR]
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- 2021
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7. Le futur des expérimentations en toxicologie.
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Gégot, Solène and Joubert, Olivier
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DRUG development ,ANIMAL development ,TRANSGENIC animals ,ANIMAL welfare ,ANIMAL experimentation - Abstract
Résumé: Le domaine de recherche de la toxicologie évolue de plus en plus, devant s'adapter aux multiples enjeux amenés par notre société actuelle. Régie par des instances réglementaires et des lois, l'expérimentation n'a plus une entière liberté dans la façon de mener ses recherches. Contrairement à une époque où l'expérimentation in vivo faisait office de gold standard , les méthodes expérimentales évoluent vers un futur sans modèles animaux. Les réglementations vont dans ce sens en étoffant les lois avec des décrets incitant le plus possible à un remplacement de ces anciennes pratiques. Ces instances invoquent l'extrapolation des données interespèces non représentatives, le coût non négligeable, les effets indésirables graves survenant lors des phases tardives du développement d'un médicament ou même après la mise sur le marché, sans oublier la question éthique du bien-être animal. Au fait des nombreuses questions posées par l'évolution de la recherche en toxicologie, il est donc essentiel de développer de nouvelles manières d'expérimenter. En se basant sur la règle des 3R (Réduire, Raffiner, Remplacer), de nouveaux modèles ont émergé. Dans un souci d'atténuer au mieux les souffrances animales et de réduire leurs utilisations, des points sont évoqués concernant la douleur, de nouvelles données d'imageries et d'explorations, ainsi que le développement des animaux transgéniques. L'arrivée des modèles in silico permet de mettre en lien les données déjà existantes et de prédire le risque toxique d'expositions à de nombreuses substances de notre environnement. Les nouvelles méthodes in vitro, concernant la culture de cellule humaine sous forme classique ou 3D, offrent des pistes d'exploration. Le développement récent d'organes sur puce nous permettrait de simuler au plus près nos organes dans leurs véritables conditions physiologiques. Le futur de la toxicologie se profile sans expérimentation animale et répond aux besoins actuels de la société. The field of toxicology research is evolving, adapting as necessary to the multiple issues raised by society today. Regulated by official bodies and numerous categories of laws, researchers can no longer conduct experiments in complete freedom. Unlike the time when in vivo experimentation was the gold standard, experimental methods are moving increasingly towards a future without animal models. Regulations are moving in this direction by fleshing out laws with decrees that encourage the replacement of these old practices insofar as possible. They invoke the extrapolation of non-representative interspecies data, non-negligible costs, and serious adverse effects occurring during the late phases of drug development or even after marketing, as well as the ethical issues of animal welfare. These various issues raised by the changes in toxicology research require the development of new ways of experimentation. New models have emerged from the 3R rule – Reduce, Refine, Replace. In an effort to reduce animal suffering and reduce their use, work has been conducted concerning pain, new imaging and exploration data, and the development of transgenic animals. The arrival of in silico models makes it possible to link existing data and to predict the toxic risk of exposure to many substances in our environment. The new in vitro methods enabling the culture of human cells in standard or 3D form offer new avenues of exploration. The recent development of organ-on-a-chip technology may allow us to simulate our organs as closely as possible in their real physiological conditions. The future of toxicology appears to reject animal experimentation while meeting the current needs of society. [ABSTRACT FROM AUTHOR]
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- 2021
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8. Părintele toxicologiei moderne românești – prof. dr. doc. farm. Nicolae I. Ioanid (1897-1990)* .
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Vlăsceanu, Gabriela-Antoaneta and Suliman, Maria-Gabriela
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PHARMACEUTICAL chemistry , *PHARMACISTS , *DRAMATIC music , *COLLEGE teachers , *FORENSIC toxicology - Abstract
Nicolae I. Ioanid was born in Tulcea, as the son of a pharmacist. He graduated from the Bucharest Faculty of Sciences, with a degree in chemistry, the Faculty of Pharmacy, and the Bucharest Conservatory of Music and Dramatic Art. He was a forensic chemist at the Forensic Institute, doctor of chemical sciences, substitute associate professor in the discipline of toxicology, professor, chief professor of toxicology, dean of the Faculty of Pharmacy (1956-1961), certified professor, head of department, doctor of pharmaceutical sciences, certified professor head of department and docent doctor. He reorganized the toxicology laboratory at the Forensic Institute. [ABSTRACT FROM AUTHOR]
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- 2021
9. NOUVELLES STRATÉGIES D'ÉVALUATION DE LA TOXICITÉ EN TOXICOLOGIE.
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TETE, Arnaud, BORTOLI, Sylvie, and COUMOUL, Xavier
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- 2023
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10. Recommandations de pratique clinique sur la prise en charge du patient adulte à présentation psychiatrique dans les structures d'urgences.
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Chauvin, A., Massoubre, C., Gil-Jardine, C., Sicot, R., Le Conte, P., Varin, L., Lefort, H., Camus, V., Martinez, M., Bied, C., Oberlin, M., Valdenaire, G., Villoing, B., Zanker, C., Lopez-Castroman, J., and Claret, P.-G.
- Abstract
Copyright of Annales Françaises de Médecine d'Urgence is the property of John Libbey Eurotext Ltd. and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)
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- 2021
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11. Dr. Sten Forshufvud - a dentist who restored a historical truth.
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Burlibasa, Mihai, Cristache, Corina Marilena, Tănase, Gabriela, Lupascu, Miruna Ana, Ionescu, Radu Gabriel, and Drafta, Sergiu
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DENTISTS ,TOXICOLOGISTS - Abstract
Copyright of dentalTarget is the property of dentalTarget and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)
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- 2022
12. Systematic comparison of transcriptomes of Caco-2 cells cultured under different cellular and physiological conditions
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Janneke Elzinga, Menno Grouls, Guido J. E. J. Hooiveld, Meike van der Zande, Hauke Smidt, and Hans Bouwmeester
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WIMEK ,Health, Toxicology and Mutagenesis ,BacGen ,Unlock ,Team Toxicology ,Caco-2 ,General Medicine ,Toxicology ,Microbiology ,3R ,Metabolism and Genomics ,Voeding, Metabolisme en Genomica ,Gut-on-a-chip ,In vitro ,Voeding ,Microbiologie ,Good in vitro method practices ,Metabolisme en Genomica ,Nutrition, Metabolism and Genomics ,MolEco ,Transcriptome ,Toxicologie ,VLAG ,Nutrition - Abstract
There is a need for standardized in vitro models emulating the functionalities of the human intestinal tract to study human intestinal health without the use of laboratory animals. The Caco-2 cell line is a well-accepted and highly characterized intestinal barrier model, which has been intensively used to study intestinal (drug) transport, host–microbe interactions and chemical or drug toxicity. This cell line has been cultured in different in vitro models, ranging from simple static to complex dynamic microfluidic models. We aimed to investigate the effect of these different in vitro experimental variables on gene expression. To this end, we systematically collected and extracted data from studies in which transcriptome analyses were performed on Caco-2 cells grown on permeable membranes. A collection of 13 studies comprising 100 samples revealed a weak association of experimental variables with overall as well as individual gene expression. This can be explained by the large heterogeneity in cell culture practice, or the lack of adequate reporting thereof, as suggested by our systematic analysis of experimental parameters not included in the main analysis. Given the rapidly increasing use of in vitro cell culture models, including more advanced (micro) fluidic models, our analysis reinforces the need for improved, standardized reporting protocols. Additionally, our systematic analysis serves as a template for future comparative studies on in vitro transcriptome and other experimental data.
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- 2023
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13. Connecting Gut Microbial Diversity with Plasma Metabolome and Fecal Bile Acid Changes Induced by the Antibiotics Tobramycin and Colistin Sulfate
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Aishwarya Murali, Varun Giri, Franziska Maria Zickgraf, Philipp Ternes, Hunter James Cameron, Saskia Sperber, Volker Haake, Peter Driemert, Hennicke Kamp, Dorothee Funk-Weyer, Shana J. Sturla, Ivonne M.C.M. Rietjens, and Bennard van Ravenzwaay
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WIMEK ,Life Science ,General Medicine ,Toxicology ,Toxicologie ,VLAG - Abstract
The diversity of microbial species in the gut has a strong influence on health and development of the host. Further, there are indications that the variation in expression of gut bacterial metabolic enzymes is less diverse than the taxonomic profile, underlying the importance of microbiome functionality, particularly from a toxicological perspective. To address these relationships, the gut bacterial composition of Wistar rats was altered by a 28 day oral treatment with the antibiotics tobramycin or colistin sulfate. On the basis of 16S marker gene sequencing data, tobramycin was found to cause a strong reduction in the diversity and relative abundance of the microbiome, whereas colistin sulfate had only a marginal impact. Associated plasma and fecal metabolomes were characterized by targeted mass spectrometry-based profiling. The fecal metabolome of tobramycin-treated animals had a high number of significant alterations in metabolite levels compared to controls, particularly in amino acids, lipids, bile acids (BAs), carbohydrates, and energy metabolites. The accumulation of primary BAs and significant reduction of secondary BAs in the feces indicated that the microbial alterations induced by tobramycin inhibit bacterial deconjugation reactions. The plasma metabolome showed less, but still many alterations in the same metabolite groups, including reductions in indole derivatives and hippuric acid, and furthermore, despite marginal effects of colistin sulfate treatment, there were nonetheless systemic alterations also in BAs. Aside from these treatment-based differences, we also uncovered interindividual differences particularly centering on the loss of Verrucomicrobiaceae in the microbiome, but with no apparent associated metabolite alterations. Finally, by comparing the data set from this study with metabolome alterations in the MetaMapTox database, key metabolite alterations were identified as plasma biomarkers indicative of altered gut microbiomes resulting from a wide activity spectrum of antibiotics.
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- 2023
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14. Toxicokinetics of Ag from Ag2S NP exposure in Tenebrio molitor and Porcellio scaber
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Zahra Khodaparast, Cornelis A.M. van Gestel, Ana Rita R. Silva, Geert Cornelis, Elma Lahive, Amaia Green Etxabe, Claus Svendsen, Marta Baccaro, Nico van den Brink, Neja Medvešček, Sara Novak, Anita Jemec Kokalj, Damjana Drobne, Kerstin Jurkschat, Susana Loureiro, and Ecology & Evolution
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WIMEK ,Bioavailability ,Soil pore water ,Materials Science (miscellaneous) ,Public Health, Environmental and Occupational Health ,Ag dissolution ,Toxicology ,Safety, Risk, Reliability and Quality ,Mealworms ,Safety Research ,Toxicologie ,VLAG ,Terrestrial isopods - Abstract
Determining the potential for accumulation of Ag from Ag2S NPs as an environmentally relevant form of AgNPs in different terrestrial organisms is an essential component of a realistic risk assessment of AgNP emissions to soils. The objectives of this study were first to determine the uptake kinetics of Ag in mealworms (Tenebrio molitor) and woodlice (Porcellio scaber) exposed to Ag2S NPs in a mesocosm test, and second, to check if the obtained toxicokinetics could be predicted by single-species bioaccumulation tests. In the mesocosms, mealworms and woodlice were exposed together with plants and earthworms in soil columns spiked with 10 μg Ag g−1 dry soil as Ag2S NPs or AgNO3. The total Ag concentrations in the biota were measured after 7, 14, and 28 days of exposure. A one-compartment model was used to calculate the Ag uptake and elimination rate constants. Ag from Ag2S NPs appeared to be taken up by the mealworms with significantly different uptake rate constants in the mesocosm compared to single-species tests (K1 = 0.056 and 1.66 g dry soil g−1 dry body weight day−1, respectively), and a significant difference was found for the Ag bioaccumulation factor (BAFk = 0.79 and 0.15 g dry soil g−1 dry body weight, respectively). Woodlice did not accumulate Ag from Ag2S NPs in both tests, but uptake from AgNO3 was significantly slower in mesocosm than in single-species tests (K1 = 0.037 and 0.26 g dry soil g−1 dry body weight day−1, respectively). Our results are of high significance because they show that single-species tests may not be a good predictor for the Ag uptake in mealworms and woodlice in exposure systems having greater levels of biological complexity. Nevertheless, single-species tests could be used as a fast screening approach to assess the potential of a substance to accumulate in biota before more complex tests are conducted.
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- 2023
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15. Le microscope et le macroscope: Conflits de perspectives disciplinaires sur les liens entre pesticides et santé au travail.
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Jouzel, Jean-Noël
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PESTICIDES ,INDUSTRIAL hygiene ,PROTECTIVE clothing ,RISK management in business ,NEURODEGENERATION ,EXPOSURE dose - Abstract
Résumé: À partir d'une enquête sociologique qualitative, cet article se propose de rendre compte de la construction historique des conflits de perspectives disciplinaires sur la question des liens entre pesticides et santé des travailleurs agricoles. Il montre comment la toxicologie, en produisant des données de dangers et d'exposition à l'échelle « microscopique » des substances actives, a structuré depuis trois quarts de siècle les modalités de l'évaluation des risques préalables à la mise sur le marché des pesticides. En objectivant, pour chaque pesticide, une dose acceptable d'exposition professionnelle et les moyens de ne pas la dépasser – notamment par l'intermédiaire du port de vêtements de protection et de mesures d'hygiène – cette source de connaissances a légitimé la notion d'usage contrôlé de ces produits. L'article montre également comment l'accumulation de données épidémiologiques mettant en évidence la surincidence de certaines pathologies chroniques cancéreuses et neurodégénératives parmi la main-d'œuvre agricole exposée a questionné, depuis la fin du siècle dernier, la fiabilité de l'évaluation des risques. Produisant, pour l'essentiel, des données « macroscopiques » sur l'effet de l'exposition des agriculteurs aux pesticides en général, les études épidémiologiques restent cependant difficiles à intégrer dans des instruments d'action publique qui font de l'autorisation de mise sur le marché leur principal levier de gestion du risque. L'article souligne que la mesure de l'exposition professionnelle aux pesticides constitue le cœur des conflits politiques et épistémiques que génère ce contraste entre les visions microscopiques et macroscopiques des effets des pesticides sur la santé de la main-d'œuvre travaillant en agriculture. This article, based on a qualitative sociological survey, aims to describe the historical construction of the conflicting disciplinary perspectives on the links between pesticides and occupational health in agriculture. It shows how toxicology, by producing hazard and exposure data at the microscopic scale of active substances, has structured the procedures for the pre-market risk assessment of pesticides since World War II. By identifying, for each pesticide, an acceptable dose of occupational exposure and the means of not exceeding it — in particular through the use of protective clothing and hygiene measures — this source of knowledge has legitimized the notion of safe use of these products. The article also shows how the collection of epidemiologic data highlighting the excess incidence of some chronic cancers and neurodegenerative diseases among the exposed agricultural workforce has raised questions about the reliability of risk assessment procedures since the end of the last century. However, since most epidemiologic studies produce macroscopic data on the effect of farmers' exposure to pesticides in general, they remain difficult to integrate into the public policy instruments that make marketing authorisations their main risk management tool. The article emphasizes that the measurement of occupational exposure to pesticides is at the heart of the political and epistemic conflicts generated by this contrast between microscopic and macroscopic views of the effects of pesticides on the health of the agricultural workforce. [ABSTRACT FROM AUTHOR]
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- 2020
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16. Gross Negligence: Impacts of Microplastics and Plastic Leachates on Phytoplankton Community and Ecosystem Dynamics
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C. Amaneesh, Shankari Anna Balan, P. S. Silpa, Ji Won Kim, Kozhumal Greeshma, A. Aswathi Mohan, Aiswarya Robert Antony, Hans-Peter Grossart, Hee-Sik Kim, and Rishiram Ramanan
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Aquatic Ecosystems ,Pollutants ,WIMEK ,Algae ,Cyanotoxins ,Ecocorona ,General Chemistry ,Plastisphere ,Toxicology ,Cyanobacteria ,Ecotoxicology ,Primary Producers ,Environmental Chemistry ,Pathogens ,Plastics ,Toxicologie - Abstract
Plastic debris is an established environmental menace affecting aquatic systems globally. Recently, microplastics (MP) and plastic leachates (PL) have been detected in vital human organs, the vascular system, and in vitro animal studies positing severe health hazards. MP and PL have been found in every conceivable aquatic ecosystem─from open oceans and deep sea floors to supposedly pristine glacier lakes and snow covered mountain catchment sites. Many studies have documented the MP and PL impacts on a variety of aquatic organisms, whereby some exclusively focus on aquatic microorganisms. Yet, the specific MP and PL impacts on primary producers have not been systematically analyzed. Therefore, this review focuses on the threats posed by MP, PL, and associated chemicals on phytoplankton, their comprehensive impacts at organismal, community, and ecosystem scales, and their endogenous amelioration. Studies on MP- and PL-impacted individual phytoplankton species reveal the production of reactive oxygen species, lipid peroxidation, physical damage of thylakoids, and other physiological and metabolic changes, followed by homo- and heteroaggregations, ultimately eventuating in decreased photosynthesis and primary productivity. Likewise, analyses of the microbial community in the plastisphere show a radically different profile compared to the surrounding planktonic diversity. The plastisphere also enriches multidrug-resistant bacteria, cyanotoxins, and pollutants, accelerating microbial succession, changing the microbiome, and thus, affecting phytoplankton diversity and evolution. These impacts on cellular and community scales manifest in changed ecosystem dynamics with widespread bottom-up and top-down effects on aquatic biodiversity and food web interactions. These adverse effects─through altered nutrient cycling─have “knock-on” impacts on biogeochemical cycles and greenhouse gases. Consequently, these impacts affect provisioning and regulating ecosystem services. Our citation network analyses (CNA) further demonstrate dire effects of MP and PL on all trophic levels, thereby unsettling ecosystem stability and services. CNA points to several emerging nodes indicating combined toxicity of MP, PL, and their associated hazards on phytoplankton. Taken together, our study shows that ecotoxicity of plastic particles and their leachates have placed primary producers and some aquatic ecosystems in peril.
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- 2022
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17. Use of Physiologically Based Kinetic Modeling-Based Reverse Dosimetry to Predict In Vivo Nrf2 Activation by EGCG and Its Colonic Metabolites in Humans
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Chen Liu, Jolijn van Mil, Annelies Noorlander, and Ivonne M.C.M. Rietjens
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reverse dosimetry ,Team Toxicology ,novel approach methodology ,General Chemistry ,Toxicology ,Nrf2 ,microbial metabolism ,gallic acid ,General Agricultural and Biological Sciences ,EGCG ,pyrogallol ,Toxicologie ,VLAG ,PBK model - Abstract
(-)-Epigallocatechin gallate (EGCG) is prone to microbial metabolism when reaching the colon. This study aimed to develop a human physiologically based kinetic (PBK) model for EGCG, with sub-models for its colonic metabolites gallic acid and pyrogallol. Results show that the developed PBK model could adequately predict in vivo time-dependent blood concentrations of EGCG after either the single or repeated oral administration of EGCG under both fasting and non-fasting conditions. The predicted in vivo blood Cmax of EGCG indicates that the Nrf2 activation is limited, while concentrations of its metabolites in the intestinal tract may reach levels that are higher than that of EGCG and also high enough to activate Nrf2 gene transcription. Taken together, combining in vitro data with a human PBK model allowed the prediction of a dose-response curve for EGCG-induced Nrf2-mediated gene expression in humans and provided insights into the contribution of gut microbial metabolites to this effect.
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- 2022
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18. Presence and risks of polycyclic aromatic hydrocarbons, dioxins and dioxin-like PCBs in dietary plant supplements as elucidated by a combined DR CALUX® bioassay and GC-HRMS based approach
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Felicia Akuamoa, Ron L. A. P. Hoogenboom, Yoran Weide, Guido van der Weg, Ivonne M. C. M. Rietjens, and Toine F. H. Bovee
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Team Organic Contaminants ,Bioassay chromatography ,Health, Toxicology and Mutagenesis ,Public Health, Environmental and Occupational Health ,Team Toxicology ,Team Bioassays & Biosensors ,General Chemistry ,General Medicine ,Toxicology ,GC/MS PAH Dioxins Dioxins ,TEQs Dietary supplements ,Toxicologie ,VLAG ,Food Science - Abstract
Plant-based dietary supplements may contain undesirable contaminants such as polycyclic aromatic hydrocarbons, dioxins and dioxin-like polychlorinated biphenyls (dl-PCBs) due to the sources of raw materials or processing methods used. The presence of these contaminants in a series of herbal supplements sold on the Ghanaian market for improving sexual performance was examined using the DR CALUX® bioassay in combination with GC-HRMS analysis. Overall, cell responses at 4 and 48 h exposure to extracts prepared without an acid-silica clean-up were relatively higher than the responses obtained from extracts prepared with an acid-silica clean-up. This indicated that the 40 supplements contained only low levels of stable aryl hydrocarbon receptor (AhR) agonists like polychlorinated dibenzo-p-dioxins and dibenzofurans (PCDD/Fs) and dl-PCBs, while some contained substantial amounts of less stable AhR-agonists. Ten supplements selected for confirmation with GC-HRMS analysis contained PCDD/Fs and dl-PCBs at levels ranging from 0.01 to 0.19 pg toxic equivalent (TEQ)/g only, while the level of the sum of 4 polycyclic aromatic hydrocarbons (Σ4PAHs) representing less stable AhR agonists, ranged from not detected (ND) to 25.5 ng/g. These concentrations were in line with the responses observed in the DR CALUX® bioassay. The concentration of PCDD/Fs and dl-PCBs corresponded to estimated daily intakes (EDIs) ranging from 0.01 to 1.20 pg TEQ/day, or 0.001 to 0.12 pg TEQ/kg bw/week for a 70 kg bw consumer, which was below the established tolerable weekly intake (TWI) of 2 pg TEQ/kg bw/week, thus indicating low concern for consumers’ health. Similarly, the EDIs based on the detected Σ4PAHs in supplements ranged from 7.2 to 111 ng/day, or 0.1 to 1.6 ng/kg bw/day, which corresponded to MOE values above 10,000, indicating a low health concern.
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- 2022
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19. Assessment of the Intestinal Absorption of Higher Olefins by the Everted Gut Sac Model in Combination with In Silico New Approach Methodologies
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Quan Shi, Juan-Carlos Carrillo, Michael G. Penman, Jason Manton, Elena Fioravanzo, Robert H. Powrie, Clifford R. Elcombe, Tilly Borsboom-Patel, Yuan Tian, Hua Shen, and Peter J. Boogaard
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Mammals ,Intestinal Absorption ,Intestine, Small ,Life Science ,Animals ,General Medicine ,Alkenes ,Toxicology ,Carbon ,Permeability ,Toxicologie ,Rats - Abstract
To reduce the number of animals and studies needed to fulfill the information requirements as required by Registration, Evaluation, Authorisation and Restriction of Chemicals (REACH) (EC no. 1907/2006), a read-across approach was used to support approximately 30 higher olefins. This study aimed to assess the absorption potential of higher olefins through the gut wall as the experimentally determined bioavailability which would strengthen the read-across hypothesis and justification, reducing the need for toxicity studies on all of the higher olefins. The absorption potential of a series of higher olefins (carbon range from 6 to 28, with five configurations of the double bond) was determined in the in vitro everted rat small intestinal sac model and subsequently ranked. In addition, in silico approaches were applied to predict the reactivity, lipophilicity, and permeability of higher olefins. In the in vitro model, everted sacs were incubated in "fed-state simulated small intestinal fluid" saturated with individual higher olefins. The sac contents were then collected, extracted, and analyzed for olefin content using gas chromatography with a flame ionization detector. The C6 to C10 molecules were readily absorbed into the intestinal sacs. Marked inter-compound differences were observed, with the amount of absorption generally decreasing with the increase in carbon number. Higher olefins with ≥C14 carbons were either not absorbed or very poorly absorbed. In the reactivity simulation study, the reactivity is well described by the position of the double bond rather than the number of carbon atoms. In the lipophilicity and permeability analysis, both parameter descriptors depend mainly on the number of carbon atoms and less on the position of the double bond. In conclusion, these new approach methodologies provide supporting information on any trends or breakpoints in intestinal uptake and a hazard matrix based on carbon number and position of the double bond. This matrix will further assist in the selection of substances for inclusion in the mammalian toxicity testing programme.
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- 2022
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20. Environnement et santé publique
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Goupil-Sormany, Isabelle, Debia, Maximilien, Glorennec, Philippe, Gonzalez, Jean-Paul, Noisel, Nolwenn, Dab, William, Chambaud, Laurent, David, Arthur, Bonvallot, Nathalie, Porcherie, Marion, Crepey, Pascal, Daubas-Letourneux, Véronique, Institut National de Santé Publique du Québec [Canada] (INSPQ), Ecole de Santé Publique de l'Université de Montréal, Université de Montréal (UdeM), Université de Rennes (UR), École des Hautes Études en Santé Publique [EHESP] (EHESP), Département Méthodes quantitatives en santé publique (METIS), Institut de recherche en santé, environnement et travail (Irset), Université d'Angers (UA)-Université de Rennes (UR)-École des Hautes Études en Santé Publique [EHESP] (EHESP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique ), ORSTOM, Conservatoire National des Arts et Métiers [CNAM] (CNAM), HESAM Université - Communauté d'universités et d'établissements Hautes écoles Sorbonne Arts et métiers université (HESAM), Laboratoire Modélisation, épidémiologie et surveillance des risques sanitaires (MESuRS), HESAM Université - Communauté d'universités et d'établissements Hautes écoles Sorbonne Arts et métiers université (HESAM)-HESAM Université - Communauté d'universités et d'établissements Hautes écoles Sorbonne Arts et métiers université (HESAM), Laboratoire d'étude et de recherche en environnement et santé (LERES), Département des sciences en santé environnementale (DEESSE), Département des sciences humaines et sociales (SHS), Centre de Recherches sur l'Action Politique en Europe (ARENES), Université de Rennes (UR)-Institut d'Études Politiques [IEP] - Rennes-École des Hautes Études en Santé Publique [EHESP] (EHESP)-Centre National de la Recherche Scientifique (CNRS), and Collectif de recherche handicap, autonomie et société inclusive (CoRHASI)
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Bruit ,Population exposée risque ,Ecosystème ,Intoxication alimentaire ,Etat santé ,Qualité eau ,Risque ,Santé publique ,Alimentation ,Réchauffement climatique ,Information ,Zoonoses ,Zoonose ,Vulnérabilité ,Appareil respiratoire ,Centre antipoison ,Evaluation ,Cancer ,One health ,Déchet ,Pays à revenu faible et intermédiaire ,Risques sanitaires ,Environnements intérieurs ,Pollution sol ,Reproduction ,Surveillance environnement ,Exposition ,Epidémiologie ,Système nerveux ,Environnement ,Système cardiovasculaire ,Exposome ,Odeur ,[SDE]Environmental Sciences ,Système immunitaire ,Rayonnement non ionisant ,Infection ,Cancers ,Participation citoyenne ,Promotion de la santé ,Prévention ,Psychologie sociale ,Déchets ,Catastrophe naturelle ,Lieu travail ,Rayonnement ionisant ,Santé environnementale ,Rayonnements ionisants ,Géographie de la santé ,Système respiratoire ,Innovation technologique ,Surveillance épidémiologique ,Sciences humaines et sociales ,Expologie ,Eaux ,Planète ,Evaluation d'impact sur la santé (EIS) ,Toxicologie ,Changement climatique ,Système reproducteur et développement ,Catastrophe industrielle ,Pathologie ,Analyse air ,Gestion risque ,Rayonnements non ionisants ,Air extérieur ,Décision ,Sols ,Environnements de travail ,Odeurs ,[SDV.SPEE]Life Sciences [q-bio]/Santé publique et épidémiologie ,Infectiologie - Abstract
International audience; Pesticides, pollution de l’air, de l’eau et des aliments, changements climatiques, menaces biologiques, chimiques, radiologiques, épidémies et inégalités environnementales de santé… Les sujets d’inquiétude quant aux conséquences de la dégradation de l’environnement sur notre santé sont nombreux et ont besoin d’être compris et analysés à l’aide des connaissances scientifiques actuelles. Unique dans le paysage éditorial et scientifique francophone, cet ouvrage présente les méthodes et approches de la santé publique environnementale d’aujourd’hui. Cette 2e édition s’enrichit de nouvelles perspectives comme la démarche « Une seule santé », le concept d’exposome, et offre une vision globale des impacts sanitaires des changements climatiques. Présentant les grands défis écologiques et les inégalités socio-environnementales de notre temps, plus de 150 auteurs s’appuient sur les données les plus récentes, établissent des objectifs au gré d’exemples illustrés et d’études de cas en Europe, en Afrique et en Amérique du Nord. Alors que les programmes axés sur la santé publique, la santé environnementale, la santé au travail et les sciences de l’environnement connaissent un engouement sans précédent, cet ouvrage est une référence pour les étudiants, enseignants, chercheurs et professionnels de ces disciplines, ainsi que pour les organisations publiques et associatives dans toute la francophonie. (R.A.)
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- 2023
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21. Les expertises dans l'affaire Lafarge ou la fabrique du doute.
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Sueur, Nicolas
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CRIMINAL law ,TOXICOLOGY ,POISONING ,LEGAL testimony ,ACTIONS & defenses (Law) - Abstract
Copyright of Canadian Bulletin of Medical History is the property of University of Toronto Press and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)
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- 2019
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22. Identification of phosphodiesterase type-5 (PDE-5) inhibitors in herbal supplements using a tiered approach and associated consumer risk
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Felicia Akuamoa, Toine F. H. Bovee, Ruud van Dam, Lilian Maro, Sebastiaan Wesseling, Jacques Vervoort, Ivonne M. C. M. Rietjens, and Ron L. A. P. Hoogenboom
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Novel Foods & Agrochains ,BU Toxicologie ,Health, Toxicology and Mutagenesis ,BU Contaminanten & Toxines ,Biochemie ,Team Toxicology ,Team Bioassays & Biosensors ,Novel Foods & Agroketens ,Toxicology ,Biochemistry ,PDE-Glo bioassay ,Gas Chromatography-Mass Spectrometry ,Sildenafil Citrate ,herbal supplement ,BU Contaminants & Toxins ,LC–MS/MS ,BU Authenticity & Bioassays ,Tandem Mass Spectrometry ,Erectile dysfunction ,BU Toxicology, Novel Foods & Agrochains ,Toxicologie ,VLAG ,PDE-5 inhibitor ,Phosphoric Diester Hydrolases ,BU Toxicology ,Public Health, Environmental and Occupational Health ,Reproducibility of Results ,General Chemistry ,General Medicine ,Phosphodiesterase 5 Inhibitors ,adulteration ,Team Natural Toxins ,BU Authenticiteit & Bioassays ,BU Toxicologie, Novel Foods & Agroketens ,Dietary Supplements ,Chromatography, Liquid ,Food Science - Abstract
The use of herbal supplements for improved sexual performance is a common practice amongst the youth and some senior citizens in Ghana. These products are considered ‘natural’ and greatly preferred over synthetic alternatives due to the assurance of little to no adverse effects by producers. However, the high rate of adulteration often compromises their safety. Forty herbal supplements, of which 25 were previously shown to result in medium to high intake of phosphodiesterase type-5 (PDE-5) inhibitors using a PDE-Glo bioassay, were further investigated using liquid chromatography–tandem mass spectrometry (LC–MS/MS) analysis to examine the reliability of the bioassay and whether the observed higher responses could be ascribed to inherent plant constituents or adulterants. Results showed significant amounts of vardenafil, tadalafil and especially sildenafil, in 2, 1 and 10 samples, respectively, with total concentration levels resulting in estimated daily intakes (EDIs) above 25 mg sildenafil equivalents with six supplements even having EDIs above 100 mg sildenafil equivalents. Only one sample contained a natural ingredient (icariin), but its concentration (0.013 mg g−1) was too low to explain the observed potency in the bioassay. The estimated concentrations of PDE-5 inhibitors in 35 supplements, according to the bioassay, were in line with those of the LC–MS/MS analysis. However, discrepancies were observed for five supplements. Further examination of one of the latter supplements using the PDE-Glo bioassay to select the positive fraction and further examination with LC–MS/MS and 1H-NMR revealed the presence of hydroxythiohomosildenafil, a sildenafil analogue not yet included in the liquid chromatography–mass spectrometry reference library. This study demonstrates the significance of applying a tiered approach, where the use of a bioassay is followed by chemical analysis of bioactive samples in order to identify unknown bioactive compounds.
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- 2022
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23. The role of endogenous versus exogenous sources in the exposome of putative genotoxins and consequences for risk assessment
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Rietjens, Ivonne M C M, Arand, Michael, Bolt, Hermann M, Bourdoux, Siméon, Hartwig, Andrea, Hinrichsen, Nils, Kalisch, Christine, Mally, Angela, Pellegrino, Gloria, Ribera, Daniel, Thatcher, Natalie, Eisenbrand, Gerhard, University of Zurich, and Rietjens, Ivonne M C M
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Life sciences ,biology ,Health, Toxicology and Mutagenesis ,Process-related contaminants ,10050 Institute of Pharmacology and Toxicology ,3005 Toxicology ,genotoxins ,exposome ,endogenous exposure ,process-related contaminants ,610 Medicine & health ,General Medicine ,Genotoxins ,Toxicology ,Risk Assessment ,Exposome ,Health ,Formaldehyde ,ddc:570 ,2307 Health, Toxicology and Mutagenesis ,Humans ,570 Life sciences ,Endogenous exposure ,Toxicology and Mutagenesis ,Acrolein ,Toxicologie ,Mutagens ,VLAG - Abstract
The “totality” of the human exposure is conceived to encompass life-associated endogenous and exogenous aggregate exposures. Process-related contaminants (PRCs) are not only formed in foods by heat processing, but also occur endogenously in the organism as physiological components of energy metabolism, potentially also generated by the human microbiome. To arrive at a comprehensive risk assessment, it is necessary to understand the contribution of in vivo background occurrence as compared to the ingestion from exogenous sources. Hence, this review provides an overview of the knowledge on the contribution of endogenous exposure to the overall exposure to putative genotoxic food contaminants, namely ethanol, acetaldehyde, formaldehyde, acrylamide, acrolein, α,β-unsaturated alkenals, glycation compounds, N-nitroso compounds, ethylene oxide, furans, 2- and 3-MCPD, and glycidyl esters. The evidence discussed herein allows to conclude that endogenous formation of some contaminants appears to contribute substantially to the exposome. This is of critical importance for risk assessment in the cases where endogenous exposure is suspected to outweigh the exogenous one (e.g. formaldehyde and acrolein).
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- 2022
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24. Protein Kinase CK2 Acts as a Molecular Brake to Control NADPH Oxidase 1 Activation and Colon Inflammation
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Liu, Dan, Marie, Jean-Claude, Pelletier, Anne-Laure, Song, Zhuoyao, Ben-Khemis, Marwa, Boudiaf, Kaouthar, Pintard, Coralie, Leger, Thibaut, Terrier, Samuel, Chevreux, Guillaume, El-Benna, Jamel, Dang, Pham My-Chan, Centre de recherche sur l'Inflammation (CRI (UMR_S_1149 / ERL_8252 / U1149)), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), DANG, Pham My-Chan, AP-HP - Hôpital Bichat - Claude Bernard [Paris], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Laboratoire de Fougères - ANSES, Agence nationale de sécurité sanitaire de l'alimentation, de l'environnement et du travail (ANSES), Institut Jacques Monod (IJM (UMR_7592)), Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), La Ligue Nationale Contre le Cancer, Comité De Paris, grant no.RS18/75-13, INSERM, Labex Inflamex, CNRS and University of Paris. 2022 CK2 Controls NOX1 Activity and Colitis 1093, and Chiffoleau, Emmanuelle
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protéine kinase ,MESH: NADPH Oxidase 1 ,MESH: Casein Kinase II ,souris ,[SDV.IMM.II]Life Sciences [q-bio]/Immunology/Innate immunity ,Mice ,MESH: Colitis ,toxicité ,Animals ,Casein Kinase II ,[SDV.IMM.II] Life Sciences [q-bio]/Immunology/Innate immunity ,Inflammation ,colon ,Hepatology ,Gastroenterology ,toxicologie ,MESH: Reactive Oxygen Species ,protein kinase ,[SDV.MHEP.HEG]Life Sciences [q-bio]/Human health and pathology/Hépatology and Gastroenterology ,MESH: Inflammatory Bowel Diseases ,Colitis ,Inflammatory Bowel Diseases ,immunity ,[SDV.MHEP.HEG] Life Sciences [q-bio]/Human health and pathology/Hépatology and Gastroenterology ,MESH: Trinitrobenzenesulfonic Acid ,Trinitrobenzenesulfonic Acid ,colite ,NADPH Oxidase 1 ,tract intestinal ,intestinal tract ,Reactive Oxygen Species ,metabolism ,immunité - Abstract
International audience; BACKGROUND & AIMS: NADPH oxidase 1 (NOX1) has emerged as a prime regulator of intestinal mucosa immunity and homeostasis. Dysregulation of NOX1 may cause inflammatory bowel disease (IBD). It is not clear how NOX1 is regulated in vivo under inflammatory conditions. We studied the role of CK2 in this process.METHODS: The NOX1 organizer subunit, NADPH oxidase organizer 1 (NOXO1), was immunoprecipitated from cytokine-treated colon epithelial cells, and bound proteins were identified by mass spectrometry analysis. Sites on NOXO1 phosphorylated by CK2 were identified by nanoscale liquid chromatography coupled to tandem mass spectrometry. NOX1 activity was determined in colon epithelial cells and colonoids in the presence or absence of CX-4945, a CK2 specific inhibitor. Acute colitis was induced by administration of trinitrobenzenesulfonic acid in mice treated or not with CX-4945. Colon tissues were analyzed by histologic examination, quantitative polymerase chain reaction, and Western blots. CK2 activity, markers of inflammation, and oxidative stress were assessed.RESULTS: We identified CK2 as a major partner of NOXO1 in colon epithelial cells under inflammatory conditions. CK2 directly binds NOXO1 at the C-terminus containing the Phox homology domain and phosphorylates NOXO1 on several sites. CX-4945 increased ROS generation by NOX1 in human colon epithelial cells and organoids. Strikingly, CK2 activity was reduced in trinitrobenzenesulfonic acid-induced acute colitis, and CX-4945 exacerbated colitis inflammation as shown by increased levels of CXCL1, ROS generation, lipid peroxidation, and colon damage.CONCLUSIONS: The ubiquitous protein kinase CK2 limits NOX1 activity via NOXO1 binding and phosphorylation in colonic epithelial cells and lessens experimental colitis. Loss of CK2 activity during acute colitis results in excessive ROS production, contributing to the pathogenesis. Strategies to activate CK2 could be an effective novel therapeutic approach in IBD.
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- 2022
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25. Towards best use and regulatory acceptance of generic physiologically based kinetic (PBK) models for in vitro-to-in vivo extrapolation (IVIVE) in chemical risk assessment
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Abdulkarim Najjar, Ans Punt, John Wambaugh, Alicia Paini, Corie Ellison, Styliani Fragki, Enrica Bianchi, Fagen Zhang, Joost Westerhout, Dennis Mueller, Hequn Li, Quan Shi, Timothy W. Gant, Phil Botham, Rémi Bars, Aldert Piersma, Ben van Ravenzwaay, and Nynke I. Kramer
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Kinetics ,Regulatory acceptance ,NAMs ,PBK models ,Health, Toxicology and Mutagenesis ,Animals ,Team Toxicology ,IVIVE ,General Medicine ,Toxicology ,Models, Biological ,Toxicologie ,Risk assessment - Abstract
With an increasing need to incorporate new approach methodologies (NAMs) in chemical risk assessment and the concomitant need to phase out animal testing, the interpretation of in vitro assay readouts for quantitative hazard characterisation becomes more important. Physiologically based kinetic (PBK) models, which simulate the fate of chemicals in tissues of the body, play an essential role in extrapolating in vitro effect concentrations to in vivo bioequivalent exposures. As PBK-based testing approaches evolve, it will become essential to standardise PBK modelling approaches towards a consensus approach that can be used in quantitative in vitro-to-in vivo extrapolation (QIVIVE) studies for regulatory chemical risk assessment based on in vitro assays. Based on results of an ECETOC expert workshop, steps are recommended that can improve regulatory adoption: (1) define context and implementation, taking into consideration model complexity for building fit-for-purpose PBK models, (2) harmonise physiological input parameters and their distribution and define criteria for quality chemical-specific parameters, especially in the absence of in vivo data, (3) apply Good Modelling Practices (GMP) to achieve transparency and design a stepwise approach for PBK model development for risk assessors, (4) evaluate model predictions using alternatives to in vivo PK data including read-across approaches, (5) use case studies to facilitate discussions between modellers and regulators of chemical risk assessment. Proof-of-concepts of generic PBK modelling approaches are published in the scientific literature at an increasing rate. Working on the previously proposed steps is, therefore, needed to gain confidence in PBK modelling approaches for regulatory use.
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- 2022
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26. Exposure to the mycotoxin deoxynivalenol reduces the transport of conjugated bile acids by intestinal Caco-2 cells
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Jingxuan Wang, Wouter Bakker, Weijia Zheng, Laura de Haan, Ivonne M. C. M. Rietjens, and Hans Bouwmeester
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Bile acid transporters ,Health, Toxicology and Mutagenesis ,General Medicine ,Mycotoxins ,Toxicology ,digestive system ,Deoxynivalenol ,Bile Acids and Salts ,Intestines ,Humans ,Caco-2 Cells ,Trichothecenes ,Conjugated bile acids ,Bile acid reabsorption ,Toxicologie ,VLAG - Abstract
Conjugated bile acids are synthesized in liver and subsequently secreted into the intestinal lumen from which they are actively reabsorbed and transported back to liver. The efficient enterohepatic circulation of conjugated bile acids is important to maintain homeostasis. The mycotoxin deoxynivalenol (DON) is a fungal secondary metabolite that contaminates cereal food. Upon human exposure, it can cause intestinal dysfunction. We explored the effects of DON exposure on the intestinal absorption of conjugated bile acids and the expression of bile acid transporters using an in vitro model based on Caco-2 cell layers grown in transwells. Our study shows that the transport rate of taurocholic acid (TCA) is decreased after 48-h pre-exposure of the Caco-2 cells to 2 µM DON, which is a realistic intestinal DON concentration. Exposure to DON downregulates expression of the genes coding for the apical sodium-dependent bile acid transporter (ASBT), the ileal bile acid-binding protein (IBABP) and the organic solute transporter α (OSTα), and it counteracts the agonist activity of Farnesoid X receptor (FXR) agonist GW4064 on these genes. In addition, the transport of ten taurine or glycine-conjugated bile acids in a physiological relevant mixture by the intestinal Caco-2 cell layers was decreased after pre-exposure of the cells to DON, pointing at a potential for DON-mediated accumulation of the conjugated bile acids at the intestinal luminal side. Together the results reveal that DON inhibits intestinal bile acid reabsorption by reducing the expression of bile acid transporters thereby affecting bile acid intestinal kinetics, leading to bile acid malabsorption in the intestine. Our study provides new insights into the hazards of DON exposure.
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- 2022
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27. The effect of alkyl substitution on the oxidative metabolism and mutagenicity of phenanthrene
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Danlei Wang, Viktoria Schramm, Jeroen Pool, Eleni Pardali, Annemarijn Brandenburg, Ivonne M. C. M. Rietjens, and Peter J. Boogaard
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Mutagenicity Tests ,Health, Toxicology and Mutagenesis ,Alkylated phenanthrene ,General Medicine ,Phenanthrenes ,Toxicology ,Rats ,Oxidative Stress ,Petroleum ,Michaelis–Menten kinetics ,Mutagenesis ,Mutagenicity ,Microsomes ,Animals ,Rat ,lipids (amino acids, peptides, and proteins) ,Polycyclic Aromatic Hydrocarbons ,Toxicologie ,Mutagens ,VLAG ,Human - Abstract
Alkyl-substituted PAHs may be present in certain petroleum-derived products and in the environment and may eventually end up in consumer products, such as foodstuffs, cosmetics and pharmaceuticals. Safety concerns over possible exposure to alkylated PAHs have emerged. Bioactivation is a prerequisite for the mutagenicity and carcinogenicity of PAHs and has been extensively studied for non-substituted PAHs, while data on the bioactivation of alkyl-substituted PAHs are scarce. The present study investigated the effect of alkyl substitution on the CYP 450-mediated metabolism of phenanthrene and eight of its alkylated congeners by quantifying metabolite formation in rat and human liver microsomal incubations. Furthermore, the mutagenicity of four selected methylated phenanthrenes was compared to that of phenanthrene using the Ames test. The obtained results support the hypothesis that alkyl substitution shifts the oxidative metabolism from the aromatic ring to the alkyl side chain. Increasing the length of the alkyl chain reduced overall metabolism with metabolic conversion for 1-n-dodecyl-phenanthrene (C12) being negligible. 1- and 9-methyl-phenanthrene, in which the methyl group generates an additional bay region-like structural motif, showed mutagenicity toward Salmonella typhimurium TA98 and TA 100, whereas phenanthrene and also 2- and 3-methyl-phenanthrene, without such an additional bay region-like structural motif, tested negative. It is concluded that the position of the alkylation affects the metabolism and resulting mutagenicity of phenanthrene with the mutagenicity increasing in cases where the alkyl substituent creates an additional bay region-like structural motif, in spite of the extra possibilities for side chain oxidation.
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- 2022
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28. In vitro–in silico-based prediction of inter-individual and inter-ethnic variations in the dose-dependent cardiotoxicity of R- and S-methadone in humans
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Miaoying Shi, Yumeng Dong, Hans Bouwmeester, Ivonne M. C. M. Rietjens, and Marije Strikwold
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Quantitative in vitro to in vivo extrapolation (QIVIVE) ,Health, Toxicology and Mutagenesis ,New approach methodologies (NAM) ,Geneesmiddelen ,Inter-individual differences ,General Medicine ,Toxicology ,Models, Biological ,Cardiotoxicity ,Kinetics ,Cytochrome P-450 Enzyme System ,Microsomes, Liver ,Physiologically based kinetic (PBK) modelling ,Humans ,Humane toxicologie ,Human-induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CM) ,Methadone ,Monte Carlo simulation ,Toxicologie ,VLAG - Abstract
New approach methodologies predicting human cardiotoxicity are of interest to support or even replace in vivo-based drug safety testing. The present study presents an in vitro–in silico approach to predict the effect of inter-individual and inter-ethnic kinetic variations in the cardiotoxicity of R- and S-methadone in the Caucasian and the Chinese population. In vitro cardiotoxicity data, and metabolic data obtained from two approaches, using either individual human liver microsomes or recombinant cytochrome P450 enzymes (rCYPs), were integrated with physiologically based kinetic (PBK) models and Monte Carlo simulations to predict inter-individual and inter-ethnic variations in methadone-induced cardiotoxicity. Chemical specific adjustment factors were defined and used to derive dose–response curves for the sensitive individuals. Our simulations indicated that Chinese are more sensitive towards methadone-induced cardiotoxicity with Margin of Safety values being generally two-fold lower than those for Caucasians for both methadone enantiomers. Individual PBK models using microsomes and PBK models using rCYPs combined with Monte Carlo simulations predicted similar inter-individual and inter-ethnic variations in methadone-induced cardiotoxicity. The present study illustrates how inter-individual and inter-ethnic variations in cardiotoxicity can be predicted by combining in vitro toxicity and metabolic data, PBK modelling and Monte Carlo simulations. The novel methodology can be used to enhance cardiac safety evaluations and risk assessment of chemicals.
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- 2022
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29. Metagenome Analysis Identifies Microbial Shifts upon Deoxynivalenol Exposure and Post-Exposure Recovery in the Mouse Gut
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Jing Jin, Chen Zhang, Xiaoxu Ren, Bowen Tai, and Fuguo Xing
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inulin supplementation ,gut microbiota ,Health, Toxicology and Mutagenesis ,metagenomic analysis ,deoxynivalenol ,spontaneous recovery ,Toxicology ,Toxicologie - Abstract
Deoxynivalenol (DON) is one of the most prevalent food-associated mycotoxins, and is known to cause a variety of adverse health effects on human and animals. Upon oral exposure, the intestine is the main target organ of DON. The current study unraveled that DON exposure (2 mg/kg bw/day or 5 mg/kg bw/day) can significantly reshape the gut microbiota in a mouse model. The study characterized the specific gut microbial strains and genes changed after DON exposure and also investigated the recovery of the microbiota upon either 2 weeks daily prebiotic inulin administration or 2 weeks recovery without intervention after termination of DON exposure (spontaneous recovery). The results obtained reveal that DON exposure causes a shift in gut microorganisms, increasing the relative abundance of Akkermansia muciniphila, Bacteroides vulgatus, Hungatella hathewayi, and Lachnospiraceae bacterium 28-4, while the relative abundance of Mucispirillum schaedleri, Pseudoflavonifractor sp. An85, Faecalibacterium prausnitzii, Firmicutes bacterium ASF500, Flavonifractor plautii, Oscillibacter sp. 1-3, and uncultured Flavonifractor sp. decreased. Notably, DON exposure enhanced the prevalence of A. muciniphila, a species considered as a potential prebiotic in previous studies. Most of the gut microbiome altered by DON in the low- and high-dose exposure groups recovered after 2 weeks of spontaneous recovery. Inulin administration appeared to promote the recovery of the gut microbiome and functional genes after low-dose DON exposure, but not after high-dose exposure, at which changes were exacerbated by inulin-supplemented recovery. The results obtained help to better understand the effect of DON on the gut microbiome, and the gut microbiota’s recovery upon termination of DON exposure.
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- 2023
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30. Advancing exposure assessment approaches to improve wildlife risk assessment
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Christy Morrissey, Clémentine Fritsch, Katharine Fremlin, William Adams, Katrine Borgå, Markus Brinkmann, Igor Eulaers, Frank Gobas, Dwayne R. J. Moore, Nico van den Brink, and Ted Wickwire
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WIMEK ,Screening-level assessment ,Exposure estimation ,Geography, Planning and Development ,Uncertainty assessment ,General Medicine ,Wildlife ,Toxicology ,Toxicologie ,VLAG ,Risk assessment ,General Environmental Science - Abstract
The exposure assessment component of a Wildlife Ecological Risk Assessment aims to estimate the magnitude, frequency, and duration of exposure to a chemical or environmental contaminant, along with characteristics of the exposed population. This can be challenging in wildlife as there is often high uncertainty and error caused by broad-based, interspecific extrapolation and assumptions often because of a lack of data. Both the US Environmental Protection Agency (USEPA) and European Food Safety Authority (EFSA) have broadly directed exposure assessments to include estimates of the quantity (dose or concentration), frequency, and duration of exposure to a contaminant of interest while considering “all relevant factors.” This ambiguity in the inclusion or exclusion of specific factors (e.g., individual and species-specific biology, diet, or proportion time in treated or contaminated area) can significantly influence the overall risk characterization. In this review, we identify four discrete categories of complexity that should be considered in an exposure assessment—chemical, environmental, organismal, and ecological. These may require more data, but a degree of inclusion at all stages of the risk assessment is critical to moving beyond screening-level methods that have a high degree of uncertainty and suffer from conservatism and a lack of realism. We demonstrate that there are many existing and emerging scientific tools and cross-cutting solutions for tackling exposure complexity. To foster greater application of these methods in wildlife exposure assessments, we present a new framework for risk assessors to construct an “exposure matrix.” Using three case studies, we illustrate how the matrix can better inform, integrate, and more transparently communicate the important elements of complexity and realism in exposure assessments for wildlife. Modernizing wildlife exposure assessments is long overdue and will require improved collaboration, data sharing, application of standardized exposure scenarios, better communication of assumptions and uncertainty, and postregulatory tracking. Integr Environ Assess Manag 2023;00:1–25.
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- 2023
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31. Gut Microbiota as Well as Metabolomes of Wistar Rats Recover within Two Weeks after Doripenem Antibiotic Treatment
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Aishwarya Murali, Franziska Maria Zickgraf, Philipp Ternes, Varun Giri, Hunter James Cameron, Saskia Sperber, Volker Haake, Peter Driemert, Hennicke Kamp, Dorothee Funk Weyer, Shana J. Sturla, Ivonne M. G. M. Rietjens, and Bennard van Ravenzwaay
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Microbiology (medical) ,WIMEK ,gut microbiome ,gut microbiota and metabolome recovery ,Toxicology ,Microbiology ,metabolomics ,Virology ,carbapenems ,repeated dose oral study ,Toxicologie ,VLAG - Abstract
An understanding of the changes in gut microbiome composition and its associated metabolic functions is important to assess the potential implications thereof on host health. Thus, to elucidate the connection between the gut microbiome and the fecal and plasma metabolomes, two poorly bioavailable carbapenem antibiotics (doripenem and meropenem), were administered in a 28-day oral study to male and female Wistar rats. Additionally, the recovery of the gut microbiome and metabolomes in doripenem-exposed rats were studied one and two weeks after antibiotic treatment (i.e., doripenem-recovery groups). The 16S bacterial community analysis revealed an altered microbial population in all antibiotic treatments and a recovery of bacterial diversity in the doripenem-recovery groups. A similar pattern was observed in the fecal metabolomes of treated animals. In the recovery group, particularly after one week, an over-compensation was observed in fecal metabolites, as they were significantly changed in the opposite direction compared to previously changed metabolites upon 28 days of antibiotic exposure. Key plasma metabolites known to be diagnostic of antibiotic-induced microbial shifts, including indole derivatives, hippuric acid, and bile acids were also affected by the two carbapenems. Moreover, a unique increase in the levels of indole-3-acetic acid in plasma following meropenem treatment was observed. As was observed for the fecal metabolome, an overcompensation of plasma metabolites was observed in the recovery group. The data from this study provides insights into the connectivity of the microbiome and fecal and plasma metabolomes and demonstrates restoration post-antibiotic treatment not only for the microbiome but also for the metabolomes. The importance of overcompensation reactions for health needs further studies., Microorganisms, 11 (2), ISSN:2076-2607
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- 2023
32. Fate and PPARγ and STATs-driven effects of the mitochondrial complex I inhibitor tebufenpyrad in liver cells revealed with multi-omics
- Author
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Thibaut Léger, Patrick Balaguer, Ludovic Le Hégarat, Valérie Fessard, Laboratoire de Fougères - ANSES, Agence nationale de sécurité sanitaire de l'alimentation, de l'environnement et du travail (ANSES), Institut de Recherche en Cancérologie de Montpellier (IRCM - U1194 Inserm - UM), CRLCC Val d'Aurelle - Paul Lamarque-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Montpellier (UM), and Chiffoleau, Emmanuelle
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Health, Toxicology and Mutagenesis ,hépatocyte ,MESH: Hepatocytes ,Adenosine Triphosphate ,cell biology ,MESH: Adenosine Triphosphate ,toxicité ,protéomique ,Waste Management and Disposal ,proteomic ,inhibiteur du complexe respiratoire mitochondrial I ,MESH: Proteasome Endopeptidase Complex ,Fatty Acids ,liver cell ,MESH: STAT3 Transcription Factor ,Pollution ,Lipids ,metabolomics ,MESH: Interleukin-6 / metabolism ,MESH: Fatty Acids ,[SDV.TOX] Life Sciences [q-bio]/Toxicology ,STAT Transcription Factors ,Liver ,[SDV.TOX]Life Sciences [q-bio]/Toxicology ,métabolomique ,toxicology ,STAT3 Transcription Factor ,Proteasome Endopeptidase Complex ,Environmental Engineering ,biologie cellulaire ,lignée cellulaire HepaRG ,mitochondrial respiratory complexe I inhibitor ,Mitochondrial Proteins ,HepaRG cell line ,hepatocyte ,Environmental Chemistry ,Animals ,Humans ,MESH: Pesticides ,Pesticides ,pesticide ,cellule hépatique ,Interleukin-6 ,toxicity ,toxicologie ,MESH: STAT Transcription Factors ,Rats ,PPAR gamma ,MESH: PPAR gamma ,Hepatocytes - Abstract
Complete proteomic datasets are available in the PRIDE partner repository (Perez-Riverol et al., 2019) under identification numbers: PXD030822 and 10.6019/PXD030822 for HepaRG cells, PXD031045 and 10.6019/PXD031045 for HepaRG culture media, PXD030887 and 10.6019/PXD030887 for PHHs, and PXD030892 and 10.6019/PXD030892 for PRHs. Metabolomic data are available in the MetaboLights repository (Haug et al., 2020) under the identification number: www.ebi.ac.uk/metabolights/MTBLS4063.; International audience; The biological effects of the pesticide and mitochondrial complex I inhibitor tebufenpyrad (TEBU) on liver cells were investigated by combining proteomics and metabolomics. Both cell culture media and cellular lysates were analyzed in dose-response and kinetic experiments on the HepaRG cell line. Responses were compared with those obtained on primary human and rat hepatocytes. A multitude of phase I and II metabolites (>80) mainly common to HepaRG cells and primary hepatocytes and an increase in metabolization enzymes were observed. Synthesis of mitochondrion and oxidative phosphorylation complex constituents, fatty acid oxidation, and cellular uptake of lipids were induced to compensate for complex I inhibition and the decrease in ATP intracellular contents caused by TEBU. Secretion of the 20 S circulating proteasome and overall inhibition of acute inflammation followed by IL-6 secretion in later stages were observed in HepaRG cells. These effects were associated with a decrease in STAT1 and STAT3 transcription factor abundances, but with different kinetics. Based on identified TEBU targets, docking experiments, and nuclear receptor reporter assays, we concluded that liver cell response to TEBU is mediated by its interaction with the PPARγ transcription factor.
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- 2023
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33. Drug Metabolism of Hepatocyte-like Organoids and Their Applicability in In Vitro Toxicity Testing
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Bouwmeester, Manon C, Tao, Yu, Proença, Susana, van Steenbeek, Frank G, Samsom, Roos-Anne, Nijmeijer, Sandra M, Sinnige, Theo, van der Laan, Luc J W, Legler, Juliette, Schneeberger, Kerstin, Kramer, Nynke I, Spee, Bart, CS_STEM, Interne geneeskunde GD, CS_Genetics, IRAS OH Toxicology, CS_STEM, Interne geneeskunde GD, CS_Genetics, IRAS OH Toxicology, and Surgery
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hepatotoxicity ,intrahepatic cholangiocyte organoids ,Organic Chemistry ,Pharmaceutical Science ,Toxicology ,Analytical Chemistry ,SDG 3 - Good Health and Well-being ,Chemistry (miscellaneous) ,Drug Discovery ,Molecular Medicine ,Physical and Theoretical Chemistry ,hepatic in vitro model ,drug-induced liver injury ,hepatocyte-like cells ,Toxicologie - Abstract
Emerging advances in the field of in vitro toxicity testing attempt to meet the need for reliable human-based safety assessment in drug development. Intrahepatic cholangiocyte organoids (ICOs) are described as a donor-derived in vitro model for disease modelling and regenerative medicine. Here, we explored the potential of hepatocyte-like ICOs (HL-ICOs) in in vitro toxicity testing by exploring the expression and activity of genes involved in drug metabolism, a key determinant in drug-induced toxicity, and the exposure of HL-ICOs to well-known hepatotoxicants. The current state of drug metabolism in HL-ICOs showed levels comparable to those of PHHs and HepaRGs for CYP3A4; however, other enzymes, such as CYP2B6 and CYP2D6, were expressed at lower levels. Additionally, EC50 values were determined in HL-ICOs for acetaminophen (24.0–26.8 mM), diclofenac (475.5–>500 µM), perhexiline (9.7–>31.5 µM), troglitazone (23.1–90.8 µM), and valproic acid (>10 mM). Exposure to the hepatotoxicants showed EC50s in HL-ICOs comparable to those in PHHs and HepaRGs; however, for acetaminophen exposure, HL-ICOs were less sensitive. Further elucidation of enzyme and transporter activity in drug metabolism in HL-ICOs and exposure to a more extensive compound set are needed to accurately define the potential of HL-ICOs in in vitro toxicity testing.
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- 2023
34. Human biomonitoring of low-level benzene exposures
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Peter J. Boogaard
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human biomonitoring ,biomarker ,Benzene ,limit value ,occupational exposure ,Toxicology ,Toxicologie - Abstract
Historically, benzene has been widely used in a large variety of applications. Occupational exposure limits (OELs) were set for benzene as it was found to be acutely toxic, causing central nervous system depression at high exposures. OELs were lowered when it was discovered that chronic exposure to benzene could cause haematotoxicity. After confirmation that benzene is a human carcinogen causing acute myeloid leukaemia and possibly other blood malignancies, OEL were further lowered. The industrial application of benzene as solvent is almost completely discontinued but it is still used as feedstock for the production of other materials, such as styrene. Occupational exposure to benzene may also occur since it is present in crude oil, natural gas condensate and a variety of petroleum products and because benzene can be formed in combustion of organic material. In the past few years, lower OELs for benzene in the range of 0.05–0.25 ppm have been proposed or were already established to protect workers from benzene-induced cancer. The skin is an important potential route of exposure and relatively more important at lower OELs. Consequently, human biomonitoring–which integrates all exposure routes–is routinely applied to control overall exposure to benzene. Several potential biomarkers have been proposed and investigated. For compliance check of the current low OELs, urinary S-phenylmercapturic acid (S-PMA), urinary benzene and blood benzene are feasible biomarkers. S-PMA appears to be the most promising biomarker but proper validation of biomarker levels corresponding to airborne benzene concentrations below 0.25 ppm are needed.
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- 2023
35. Compensatory responses differ between parental tasks in a songbird species
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Matteo Schiavinato, Matteo Griggio, Andrea A. Pilastro, and Davide Baldan
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partial compensation ,negotiation ,parental task ,parental care ,Animal Science and Zoology ,Spanish sparrow ,Toxicology ,nest defence ,Ecology, Evolution, Behavior and Systematics ,Toxicologie - Abstract
In species with biparental care, the amount of care devoted to offspring is affected by the negotiation rules that the parents adopt. Theoretical models predict that biparental care can be evolutionarily stable if a decrease in parental investment by one parent is only partially compensated by its partner. However, empirical studies have found substantial variability in compensatory behaviour and have mainly used nesting provisioning as a single measure of parental effort. In this study, we investigated parental compensatory behaviour for two parental tasks, offspring provisioning and nest defence. These two tasks are likely characterized by different levels of risk as well as different cost and benefit functions for the parents, which may affect the expected level of compensatory responses. We experimentally widowed (by temporarily removing one parent) male or female Spanish sparrows, Passer hispaniolensis, and measured their compensatory responses to offspring provisioning and nest defence (after predator presentation of green whip snake, Hierophis viridiflavus, models). Parents differed in their compensatory responses in relation to parental task and sex: both sexes partially compensated for offspring provisioning, but females compensated by a larger degree than males. For predator defence, males instead decreased defence behaviour by increasing latency and reducing the number of attacks, while females did not change their behaviour when caring alone. This within-individual comparison indicates that parents adjust their compensatory behaviour according to parental task. We discuss how these differences could arise due to different costs and benefits of extra investments.
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- 2023
36. Effects of xenobiotics on gut microbiota and related bile acid metabolism
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Weijia Zheng, Wageningen University, I.M.C.M. Rietjens, J. Wang, and M. Jin
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Life Science ,Toxicology ,Toxicologie ,VLAG - Published
- 2023
37. Moving beyond standard toxicological metrics : The effect of diclofenac on planktonic host-parasite interactions
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Nandini Vasantha Raman, Alena S. Gsell, Themistoklis Voulgarellis, Nico W. van den Brink, Lisette N. de Senerpont Domis, Aquatic Ecology (AqE), and AKWA
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WIMEK ,Diclofenac ,Indirect effects ,Health, Toxicology and Mutagenesis ,Direct effects ,Aquatic Science ,Host-parasite interaction ,Toxicology ,Toxicologie ,Chytrid - Abstract
Pharmaceuticals are increasingly released into surface waters and therefore ubiquitous in aquatic systems. While pharmaceuticals are known to influence species interactions, their effect on host-parasite interactions is still underexplored despite potential ecosystem-level consequences. Here, we ask whether diclofenac, a widely used non-steroid anti-inflammatory drug, affects the interaction between a phytoplankton host (Staurastrum sp.; green alga) and its obligate fungal parasite (Staurastromyces oculus; chytrid fungus). We hypothesized that the effect of increasing diclofenac concentration on the host-parasite system depends on parasite exposure. We assessed acute and chronic effects of a wide range of diclofenac concentrations (0–150 mg/L) on host and parasite performance using a replicated long gradient design in batch cultures. Overall system response summarizing parameters related to all biotic components in an experimental unit i.e., number of bacteria and phytoplankton host cells along with photosynthetic yield (a measure of algal cell fitness), depended on diclofenac concentration and presence/absence of parasite. While host standing biomass decreased at diclofenac concentrations >10 mg/L in non-parasite-exposed treatments, it increased at ≥10 mg/L in parasite-exposed treatments since losses due to infection declined. During acute phase (0–48 h), diclofenac concentrations 10 mg/L in non-parasite-exposed cultures, while it was overall close to zero in parasite-exposed cultures. Our results suggest that chytrid parasites are more sensitive to diclofenac than their host, allowing a window of opportunity for growth of phytoplankton hosts, despite exposure to a parasite. Our work provides a first understanding about effects of a pharmaceutical on a host-parasite interaction beyond those defined by standard toxicological metrics.
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- 2023
38. Use of new approach methodologies to study the developmental toxicity of polycyclic aromatic hydrocarbons
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Toxicology ,Toxicologie ,VLAG - Published
- 2023
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39. Mercury-Modulated Immune Responses in Arctic Barnacle Goslings (Branta leucopsis) upon a Viral-Like Immune Challenge
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Biyao Han, Hans van den Berg, Maarten J.J.E. Loonen, Rafael Mateo, and Nico W. van den Brink
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WIMEK ,mercury ,avian ,arctic ,barnacle goose (Branta leucopsis) ,exposure and effect ,immune toxicity ,Environmental Chemistry ,General Chemistry ,Toxicology ,Toxicologie ,VLAG - Abstract
Historical mining activities in Svalbard (79°N/12°E) have caused local mercury (Hg) contamination. To address the potential immunomodulatory effects of environmental Hg on Arctic organisms, we collected newborn barnacle goslings (Branta leucopsis) and herded them in either a control or mining site, differing in Hg levels. An additional group at the mining site was exposed to extra inorganic Hg(II) via supplementary feed. Hepatic total Hg concentrations differed significantly between the control (0.011 ± 0.002 mg/kg dw), mine (0.043 ± 0.011 mg/kg dw), and supplementary feed (0.713 ± 0.137 mg/kg dw) gosling groups (average ± standard deviation). Upon immune challenge with double-stranded RNA (dsRNA) injection, endpoints for immune responses and oxidative stress were measured after 24 h. Our results indicated that Hg exposure modulated the immune responses in Arctic barnacle goslings upon a viral-like immune challenge. Increased exposure to both environmental as well as supplemental Hg reduced the level of natural antibodies, suggesting impaired humoral immunity. Hg exposure upregulated the expression of proinflammatory genes in the spleen, including inducible nitric oxide synthase (iNOS) and interleukin 18 (IL18), suggesting Hg-induced inflammatory effects. Exposure to Hg also oxidized glutathione (GSH) to glutathione disulfide (GSSG); however, goslings were capable of maintaining the redox balance by de novo synthesis of GSH. These adverse effects on the immune responses indicated that even exposure to low, environmentally relevant levels of Hg might affect immune competence at the individual level and might even increase the susceptibility of the population to infections.
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- 2023
40. Letter to the Editors regarding '10% body weight (gain) change as criterion for the maximum tolerated dose : A critical analysis'
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Sir Colin L. Berry, Samuel M. Cohen, J. Christopher Corton, Joao Lauro Viana de Camargo, Gerhard Eisenbrand, Shoji Fukushima, Helmut Greim, Klaus Weber, Ivonne M.C.M. Rietjens, and Christian Strupp
- Subjects
WIMEK ,Life Science ,General Medicine ,Toxicology ,Toxicologie ,VLAG - Published
- 2023
41. Gut microbiota-mediated metabolism of green tea catechins and the biological consequences : An updated review
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Chen Liu, Ren-You Gan, Daiwen Chen, Liang Zheng, Siew Bee Ng, and Ivonne M. C. M. Rietjens
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in vitro fermentation models ,WIMEK ,beneficial effects ,gut microbiota ,low-molecular-weight metabolites ,General Medicine ,intra- and inter-individual differences ,Toxicology ,Industrial and Manufacturing Engineering ,green tea catechins ,Toxicologie ,Food Science ,VLAG - Abstract
Multiple beneficial effects have been attributed to green tea catechins (GTCs). However, the bioavailability of GTCs is generally low, with only a small portion directly absorbed in the small intestine. The majority of ingested GTCs reaches the large intestinal lumen, and are extensively degraded via biotransformation by gut microbiota, forming many low-molecular-weight metabolites such as phenyl-γ-valerolactones, phenolic acids, butyrate, and acetate. This process not only improves the overall bioavailability of GTC-derived metabolites but also enriches the biological activities of GTCs. Therefore, the intra- and inter-individual differences in human gut microbiota as well as the resulting biological contribution of microbial metabolites are crucial for the ultimate health benefits. In this review, the microbial degradation of major GTCs was characterized and an overview of the in vitro models used for GTC metabolism was summarized. The intra- and inter-individual differences of human gut microbiota composition and the resulting divergence in the metabolic patterns of GTCs were highlighted. Moreover, the potential beneficial effects of GTCs and their gut microbial metabolites were also discussed. Overall, the microbial metabolites of GTCs with higher bioavailability and bioactive potency are key factors for the observed beneficial effects of GTCs and green tea consumption.
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- 2023
42. Toxicokinetics and bioaccumulation of silver sulfide nanoparticles in benthic invertebrates in an indoor stream mesocosm
- Author
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Patrícia V. Silva, Ana Rita R. Silva, Nathaniel J. Clark, Joanne Vassallo, Marta Baccaro, Neja Medvešček, Magdalena Grgić, Abel Ferreira, Martí Busquets-Fité, Kerstin Jurkschat, Anastasios G. Papadiamantis, Victor Puntes, Iseult Lynch, Claus Svendsen, Nico W. van den Brink, Richard D. Handy, Cornelis A.M. van Gestel, Susana Loureiro, and Ecology & Evolution
- Subjects
History ,Environmental Engineering ,WIMEK ,Polymers and Plastics ,Toxicology ,Pollution ,Single-species tests ,Industrial and Manufacturing Engineering ,Sediments ,Uptake and elimination ,Environmental Chemistry ,SDG 14 - Life Below Water ,Business and International Management ,Waste Management and Disposal ,Exposure routes ,Toxicologie ,VLAG ,Nanomaterials ,Risk assessment - Abstract
Mesocosms allow the simulation of environmentally relevant conditions and can be used to establish more realistic scenarios of organism exposure to nanoparticles. An indoor mesocosm experiment simulating an aquatic stream ecosystem was conducted to assess the toxicokinetics and bioaccumulation of silver sulfide nanoparticles (Ag2S NPs) and AgNO3 in the freshwater invertebrates Girardia tigrina, Physa acuta and Chironomus riparius, and determine if previous single-species tests can predict bioaccumulation in the mesocosm. Water was daily spiked at 10 μg Ag L−1. Ag concentrations in water and sediment reached values of 13.4 μg Ag L−1 and 0.30 μg Ag g−1 in the Ag2S NP exposure, and 12.8 μg Ag L−1 and 0.20 μg Ag g−1 in the AgNO3. Silver was bioaccumulated by the species from both treatments, but with approximately 1.5, 3 and 11 times higher body Ag concentrations in AgNO3 compared to Ag2S NP exposures in snails, chironomids and planarians, respectively. In the Ag2S NP exposures, the observed uptake was probably of the particulate form. This demonstrates that this more environmentally relevant Ag nanoform may be bioavailable for uptake by benthic organisms. Interspecies interactions likely occurred, namely predation (planarians fed on chironomids and snails), which somehow influenced Ag uptake/bioaccumulation, possibly by altering organisms´ foraging behaviour. Higher Ag uptake rate constants were determined for AgNO3 (0.64, 80.4 and 1.12 Lwater g−1organism day−1) than for Ag2S NPs (0.05, 2.65 and 0.32 Lwater g−1organism day−1) for planarians, snails and chironomids, respectively. Biomagnification under environmentally realistic exposure seemed to be low, although it was likely to occur in the food chain P. acuta to G. tigrina exposed to AgNO3. Single-species tests generally could not reliably predict Ag bioaccumulation in the more complex mesocosm scenario. This study provides methodologies/data to better understand exposure, toxicokinetics and bioaccumulation of Ag in complex systems, reinforcing the need to use mesocosm studies to improve the risk assessment of environmental contaminants, specifically NPs, in aquatic environments.
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- 2023
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43. High resolution mass spectrometric suspect screening, wide-scope target analysis of emerging contaminants and determination of legacy pollutants in adult black-tailed godwit Limosa limosa limosa in the Netherlands – A pilot study
- Author
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P. Movalli, K. Biesmeijer, G. Gkotsis, N. Alygizakis, M.C. Nika, K. Vasilatos, M. Kostakis, N.S. Thomaidis, P. Oswald, M. Oswaldova, J. Slobodnik, N. Glowacka, J.C.E.W. Hooijmeijer, R.A. Howison, R.W.R.J. Dekker, N. van den Brink, T. Piersma, Conservation Ecology Group, and Piersma group
- Subjects
Emerging contaminants ,Environmental Engineering ,WIMEK ,PBDEs ,Health, Toxicology and Mutagenesis ,Public Health, Environmental and Occupational Health ,PCDDs/PCDFs/dl-PCBs ,General Medicine ,General Chemistry ,Suspect screening ,Wide-scope target analysis ,Toxicology ,Pollution ,Black-tailed godwit ,Environmental Chemistry ,Limosa limosa limosa ,Toxicologie ,VLAG - Abstract
The Dutch breeding population of the black-tailed godwit Limosa limosa limosa has declined substantially over recent decades; the role of contaminants is unknown. We analysed liver samples from 11 adult birds found dead on their breeding grounds in SW Friesland 2016–2020, six from extensive, herb-rich grasslands, five from intensive grasslands. We carried out LC and GC wide-scope target analysis of more than 2400 substances, LC suspect screening for more than 60,000 substances, target analysis for Cd, Hg, Ni and Pb, organo-phosphate flame retardants (OPFRs), dechlorane plus compounds and selected polybrominated diphenyl ether flame retardants (PBDEs), and bioassay for polybrominated dibenzo-p-dioxins and dibenzofurans (PBDDs/PDBFs) and dioxin-like polychlorinated biphenyls (dl-PCBs). Residues of 29 emerging contaminants (ECs) were determined through wide-scope target analysis. Another 20 were tentatively identified through suspect screening. These contaminants include industrial chemicals (personal care products, surfactants, PAHs and others), plant protection products (PPPs) and pharmaceuticals and their transformation products. Total contaminant load detected by wide-scope target analysis ranged from c. 155 to c. 1400 ng g−1 and was generally lower in birds from extensive grasslands. Heatmaps suggest that birds from intensive grasslands have a greater mix and higher residue concentrations of PPPs, while birds from extensive grasslands have a greater mix and higher residue concentrations of per- and polyfluoroalkyl substances (PFAS). All four metals and two OPFRs were detected. All tested PBDEs were below the respective LODs. Bioassay revealed presence of PBDDs, PBDFs and dl-PCBs. Further research is required to elucidate potential health risks to godwits and contaminant sources.
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- 2023
44. Physiologically based kinetic modeling of senecionine N-oxide in rats as a new approach methodology to define the effects of dose and endpoint used on relative potency values of pyrrolizidine alkaloid N-oxides
- Author
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Widjaja, Frances, Zheng, Liang, Wesseling, Sebastiaan, and Rietjens, Ivonne M.C.M.
- Subjects
Pharmacology ,WIMEK ,Toxicology ,physiologically based kinetic modeling ,relative potency value ,7-GS-DHP ,senecionine N-oxide ,Pharmacology (medical) ,rat ,senecionine ,pyrrole-protein adducts ,Toxicologie ,VLAG - Abstract
Over 1,000 pyrrolizidine alkaloids (PAs) and their N-oxides (PA-N-oxides) occur in 3% of all flowering plants. PA-N-oxides are toxic when reduced to their parent PAs, which are bioactivated into pyrrole intermediates that generate protein- and DNA-adducts resulting in liver toxicity and carcinogenicity. Literature data for senecionine N-oxide in rats indicate that the relative potency (REP) value of this PA-N-oxide compared to its parent PA senecionine varies with the endpoint used. The first endpoint was the ratio between the area under the concentration-time curve (AUC) for senecionine upon dosing senecionine N-oxide or an equimolar dose of senecionine, while the second endpoint was the ratio between the amount for pyrrole-protein adducts formed under these conditions. This study aimed to investigate the mode of action underlying this endpoint dependent REP value for senecionine N-oxide with physiologically based kinetic (PBK) modeling. Results obtained reveal that limitation of 7-GS-DHP adduct formation due to GSH depletion, resulting in increased pyrrole-protein adduct formation, occurs more likely upon high dose oral PA administration than upon an equimolar dose of PA-N-oxide. At high dose levels, this results in a lower REP value when based on pyrrole-protein adduct levels than when based on PA concentrations. At low dose levels, the difference no longer exists. Altogether, the results of the study show how the REP value for senecionine N-oxide depends on dose and endpoint used, and that PBK modeling provides a way to characterize REP values for PA-N-oxides at realistic low dietary exposure levels, thus reducing the need for animal experiments.
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- 2023
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45. Unravelling the functional dynamics between the human gut microbiome and intestinal inflammatory responses
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Grouls, Menno, Wageningen University, H. Bouwmeester, I.M.C.M. Rietjens, and M. van der Zande
- Subjects
Life Science ,Team Toxicology ,Toxicology ,Toxicologie ,VLAG - Published
- 2023
- Full Text
- View/download PDF
46. Potential human health effects following exposure to nano- and microplastics, lessons learned from nanomaterials
- Author
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Brouwer, Hugo, van Oijen, Femke L.N., and Bouwmeester, Hans
- Subjects
microplastics ,PBK models ,uptake ,toxicity ,Nanoplastics ,Toxicology ,Toxicologie ,VLAG ,in vitro models - Abstract
A substantial part of the plastic produced worldwide ends up in the environment and degrades into nano- and microplastics. The particles are ubiquitously present in the air and enter the food production chain as contaminants. Ingestion of nano- and microplastics present in food and drinking water, or those present in swallowed lung mucus that contain trapped particles, represent the main route of human exposure. Yet much remains to be studied on the intestinal uptake by humans and the potential this exposure has to result in adverse health effects. Here we review the current knowledge and relate this to lessons learned from the field of nanotoxicology. We discuss how in vitro and in silico approaches can be used to support the risk assessment of nano- and microplastics.
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- 2023
- Full Text
- View/download PDF
47. Use of new approach methodologies to study the developmental toxicity of polycyclic aromatic hydrocarbons
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Fang, Jing, Wageningen University, I.M.C.M. Rietjens, P.J. Boogaard, and L. Kamelia
- Subjects
Life Science ,Toxicology ,Toxicologie ,VLAG - Published
- 2023
48. Mogelijke risico’s van vislood in het aquatische milieu
- Subjects
Environmental Risk Assessment ,Aquatic Ecology and Water Quality Management ,WIMEK ,Aquatische Ecologie en Waterkwaliteitsbeheer ,Toxicology ,Toxicologie ,VLAG - Abstract
Stichting Gezond Water (SGW) approached the Science Shop of the WUR in 2020 with the question to investigate the risks of lost/released fishing lead to the aquatic environment. Since both professional and recreational fishing activities are very abundant in the Netherlands, and can occur on rather fixed locations lost lead accumulates locally. The use of fishing lead is officially subject to licensing under the Water Act, but this is not enforced by the responsible authorities. In 2021, the European body ECHA, as the authority responsible for regulating chemicals, submitted a proposal to phase out the use of lead in hunting and fishing. The aim is to reduce lead emissions to the environment and significantly reduce the risk of (direct and indirect) negative effects of lead on humans and ecosystems. The Commission will make a decision in 2023. -To delineate the interpretation of the experimental phase in this project on possible risks of fishing lead on the aquatic environment, literature research was conducted on the possible annual amount of fishing lead entering the environment via angling, measurements of concentrations of dissolved lead in Dutch surface water, and effect concentrations of lead in toxicity studies. Available data from various measurement sites show that the annual average throughout the Netherlands is below the environmental quality requirement (JG-MKE) of 1.2 µg/L free-dissolved lead, only sporadically has a measurement value above 1.2 µg/L been reported. In comparison, Dutch stormwater has an average lead concentration of 0.9 µg/L. Aquatic snails appear to be the most sensitive aquatic animals to dissolved lead, with a limit value of 12 μg/L below which no long-term effects are found. Moreover, lead toxicity appears to depend on certain water conditions, such as suspended solids in the water column, water hardness and pH. A previous experimental emission study with 4 lead pellets in sediment-water systems showed that lead concentrations above the JG-MKE can occur at neutral pH. The emission study with lead pellets was taken as a starting point for the experimental project phase. A dose-effect relationship was investigated with water snails, with 4 different densities of 3 mm split lead sinkers (0, 4, 20, 100 lead sinkers per jar containing 1 liter of water) both with and without a layer of 2 cm of fine sediment. After 4 weeks of lead incubation, snails were exposed for yet another 4 weeks. Dissolved lead concentrations (filtered over 45 μm) were also above the JG-MKE in the present experiment with 4 leads per liter of water in test systems without sediment, but no significant effect on mortality or growth on the (sub-)adult Physella acuta was detected. In test systems with sediment, most of the released lead was bound to sediment, but at 20 sinkers per liter of water in all replicates, dissolved lead concentrations were above the JG-MKE after 56 days. The water snail Physella acuta experienced no effects of lead on mortality, but compared to the control group, snail growth was significantly lower at 4 lead sinkers per jar of 1 liter of water. This corresponds to 108 cm2 of lead object per m2 of sediment surface area (1.1% of bottom surface area is lead). The emission rate of split lead on sediment was determined to be 3.1-3.8 mg/cm2/yr (0.26% of fish lead per year). The results of this laboratory study indicate that at the lowest density tested (lead sinkers covering 1.1% of bottom surface), lost sinkers on the water bottom surface in stagnant water pose an environmental risk. Lead densities in this study were well above those at typical fish sites (England, Wales, USA). Lead emission risks could be further tested on juvenile snails that experience greater growth than the sub-adult individuals currently used. The realistic risk to aquatic animals from dissolved lead released from sinkers in Dutch water systems is still difficult to estimate. For this, more insight is needed into, for example, the density of sinkers at popular fish sites, the extent to which sinkers stay at the sediment surface, the dilution factor (flow rate of water), the sedimentation rate of suspended solids (covering sinkers), and the influence of dredging. The area of lead objects at locations where there is a lot of recreational fishing activity seems not (yet) to be identified in the Netherlands, and should be further investigated in view of the decades-long lead backlog already present in the environment.
- Published
- 2023
- Full Text
- View/download PDF
49. Direct addition of flavors, including taste and flavor modifiers
- Author
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Ivonne M.C.M. Rietjens, Samuel M. Cohen, Gerhard Eisenbrand, Shoji Fukushima, Nigel J. Gooderham, F. Peter Guengerich, Stephen S. Hecht, Thomas J. Rosol, Matthew J. Linman, Christie L. Harman, and Sean V. Taylor
- Subjects
natural flavoring complexes ,exposure ,risk assessment ,toxicity ,safety evaluation ,Toxicology ,Flavor ,food flavorings ,Toxicologie ,VLAG - Abstract
The addition of flavorings to food and beverages provides practically unlimited opportunities for innovation, for maintaining and enhancing palatability, and is one essential element of a stable supply of nutritious consumer products. A safety evaluation by the Flavor and Extract Manufacturers Association (FEMA) Expert Panel provides a pathway for flavor producers and users to achieve regulatory authority to use for substances under the conditions of intended use as a flavoring. This chapter describes the factors that contribute to the safety assessment process that is conducted by the Expert Panel, and provides examples of specific flavorings and types of flavorings that are considered. The chapter also describes future issues and opportunities likely to be encountered within the context of the FEMA generally recognized as safe assessment of flavorings.
- Published
- 2023
- Full Text
- View/download PDF
50. The effects of hexabromocyclododecane on the transcriptome and hepatic enzyme activity in three human HepaRG-based models
- Author
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Proença, Susana, van Sabben, Nick, Legler, Juliette, Kamstra, Jorke H, Kramer, Nynke I, IRAS OH Toxicology, Dep Population Health Sciences, IRAS OH Toxicology, and Dep Population Health Sciences
- Subjects
Thyroid hormones ,PXR ,HBCD ,Sandwich ,HepaRG ,Spheroids ,Toxicology ,Toxicologie - Abstract
The disruption of thyroid hormone homeostasis by hexabromocyclododecane (HBCD) in rodents is hypothesized to be due to HBCD increasing the hepatic clearance of thyroxine (T4). The extent to which these effects are relevant to humans is unclear. To evaluate HBCD effects on humans, the activation of key hepatic nuclear receptors and the consequent disruption of thyroid hormone homeostasis were studied in different human hepatic cell models. The hepatoma cell line, HepaRG, cultured as two-dimensional (2D), sandwich (SW) and spheroid (3D) cultures, and primary human hepatocytes (PHH) cultured as sandwich were exposed to 1 and 10 mu M HBCD and characterized for their transcriptome changes. Pathway enrichment analysis showed that 3D models, followed by SW, had a stronger transcriptome response to HBCD, which is explained by the higher expression of hepatic nuclear receptors but also greater accumulation of HBCD measured inside cells in these models. The Pregnane X receptor pathway is one of the pathways most upregulated across the three hepatic models, followed by the constitutive androstane receptor and general hepatic nuclear receptors pathways. Lipid metabolism pathways had a downregulation tendency in all exposures and in both PHH and the three cultivation modes of HepaRG. The activity of enzymes related to PXR/CAR induction and T4 metabolism were evaluated in the three different types of HepaRG cultures exposed to HBCD for 48 h. Reference inducers, rifampicin and PCB-153 did affect 2D and SW HepaRG cultures' enzymatic activity but not 3D. HBCD did not induce the activity of any of the studied enzymes in any of the cell models and culture methods. This study illustrates that for nuclear receptormediated T4 disruption, transcriptome changes might not be indicative of an actual adverse effect. Clarification of the reasons for the lack of translation is essential to evaluate new chemicals' potential to be thyroid hormone disruptors by altering thyroid hormone metabolism.
- Published
- 2023
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