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5. AOP Report: An Upstream Network for Reduced Androgen Signaling Leading to Altered Gene Expression of Androgen Receptor–Responsive Genes in Target Tissues.

Author

Draskau, Monica K., Rosenmai, Anna K., Bouftas, Nora, Johansson, Hanna K. L., Panagiotou, Eleftheria M., Holmer, Marie L., Elmelund, Emilie, Zilliacus, Johanna, Beronius, Anna, Damdimopoulou, Pauliina, van Duursen, Majorie, and Svingen, Terje

Subjects
REPRODUCTIVE toxicology, ENVIRONMENTAL toxicology, ENDOCRINE disruptors, ENVIRONMENTAL chemistry, GENE targeting
Abstract

Adverse outcome pathways (AOPs) can aid with chemical risk assessment by providing plausible links between chemical activity at the molecular level and effect outcomes in intact organisms. Because AOPs can be used to infer causality between upstream and downstream events in toxicological pathways, the AOP framework can also facilitate increased uptake of alternative methods and new approach methodologies to help inform hazard identification. However, a prevailing challenge is the limited number of fully developed and endorsed AOPs, primarily due to the substantial amount of work required by AOP developers and reviewers. Consequently, a more pragmatic approach to AOP development has been proposed where smaller units of knowledge are developed and reviewed independent of full AOPs. In this context, we have developed an upstream network comprising key events (KEs) and KE relationships related to decreased androgen signaling, converging at a nodal KE that can branch out to numerous adverse outcomes (AOs) relevant to androgen‐sensitive toxicological pathways. Androgen signaling represents an extensively studied pathway for endocrine disruption. It is linked to numerous disease outcomes and can be affected by many different endocrine‐disrupting chemicals. Still, pathways related to disrupted androgen signaling remain underrepresented in the AOP‐wiki, and endorsed AOPs are lacking. Given the pivotal role of androgen signaling in development and function across vertebrate taxa and life stages of both sexes, this upstream AOP network serves as a foundational element for developing numerous AOPs. By connecting the upstream network with various downstream AOs, encompassing different species, it can also facilitate cross‐species extrapolations for hazard and risk assessment of chemicals. Environ Toxicol Chem 2024;43:2329–2337. © 2024 The Author(s). Environmental Toxicology and Chemistry published by Wiley Periodicals LLC on behalf of SETAC. [ABSTRACT FROM AUTHOR]

Published
2024
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6. Fulfilling the criteria for CLP classification: the implications for substances under the EU chemicals legislation.

Author

Kättström, Diana, Beronius, Anna, af Gennäs, Urban Boije, Rudén, Christina, and Ågerstrand, Marlene

Subjects
HAZARDOUS substances, OZONE layer, CARCINOGENICITY, MANUFACTURING industries, HAZARDS
Abstract

The CLP mandates manufacturers and importers to classify substances and mixtures according to hazard criteria, with notifications submitted to the European Chemicals Agency (ECHA). Substances meeting hazard criteria must be appropriately labelled and packaged to communicate hazards effectively. The CLP establishes hazard classification criteria but does not independently prohibit or restrict the use of hazardous chemicals. Instead, it serves as a basis for regulatory obligations in other specific regulations. This study investigates the regulatory implications of meeting hazard criteria under the CLP across EU regulations and directives listed in EU Chemicals Legislation Finder (EUCLEF). The results show that fulfilling criteria for human health hazard classes trigger regulatory obligations in the highest number of regulations/directives, with carcinogenicity, mutagenicity, and reproductive toxicity (CMR) leading to obligations in 19 of 20 pieces of legislation linked to the CLP. Conversely, physical, environmental, and ozone layer hazards are associated with fewer regulations and directives, and lead to fewer prohibitions. The study underscores the pivotal role of the CLP in EU chemical legislation and the need for coherence and consistency across regulations. While regulatory obligations are primarily aimed at substances meeting hazard criteria, the variability in self-classification notifications and limitations in harmonized classification processes were observed. Moreover, the complexity of the regulatory structure poses challenges for stakeholders and policymakers, including inconsistencies, compliance difficulties, and the need for frequent revisions. Addressing these challenges is critical for enhancing regulatory effectiveness and ensuring a more coherent and harmonized approach to chemical management in the EU. [ABSTRACT FROM AUTHOR]

Published
2024
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9. Enhanced identification of endocrine disruptors through integration of science-based regulatory practices and innovative methodologies: The MERLON Project

Author

Svingen, Terje, primary, Andersson, Anna-Maria, additional, Angelova, Julianna, additional, Axelstad, Marta, additional, Bakker, Julie, additional, Baumann, Lisa, additional, Beronius, Anna, additional, Bouftas, Nora, additional, Chalmel, Frederic, additional, Christiansen, Sofie, additional, Cornil, Charlotte, additional, Damdimopoulou, Pauliina, additional, Deepika, Deepika, additional, Dollé, Martijn E. T., additional, Draskau, Monica Kam, additional, Fischer, Margit Bistrup, additional, Hagen, Casper P., additional, Hessel, Ellen, additional, Holmer, Marie Louise, additional, Hughes, Samantha, additional, Jensen, Genon, additional, Johansson, Hanna Katarina Lilith, additional, Juul, Anders, additional, Kumar, Vikas, additional, Kumar, Saurav, additional, Lardenois, Aurélie, additional, Main, Katharina M., additional, Mazaud-Guittot, Severine, additional, Moe, S. Jannicke, additional, Mola, Gylli, additional, Parent, Anne-Simone, additional, Pineda, Rafael, additional, Rolland, Antoine, additional, Rosenmai, Anna Kjerstine, additional, Song, You, additional, Suglia, Antonio, additional, Tena-Sempere, Manuel, additional, Wehrli, Lydia, additional, Zilliacus, Johanna, additional, and van Duursen, Majorie, additional

Published
2024
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12. A proposed framework for the systematic review and integrated assessment (SYRINA) of endocrine disrupting chemicals

Author

Vandenberg, Laura N, Ågerstrand, Marlene, Beronius, Anna, Beausoleil, Claire, Bergman, Åke, Bero, Lisa A, Bornehag, Carl-Gustaf, Boyer, C Scott, Cooper, Glinda S, Cotgreave, Ian, Gee, David, Grandjean, Philippe, Guyton, Kathryn Z, Hass, Ulla, Heindel, Jerrold J, Jobling, Susan, Kidd, Karen A, Kortenkamp, Andreas, Macleod, Malcolm R, Martin, Olwenn V, Norinder, Ulf, Scheringer, Martin, Thayer, Kristina A, Toppari, Jorma, Whaley, Paul, Woodruff, Tracey J, and Rudén, Christina

Subjects
Epidemiology, Health Sciences, Estrogen, Prevention, Generic health relevance, Good Health and Well Being, Animals, Endocrine Disruptors, Environmental Exposure, Environmental Pollutants, Humans, Models, Theoretical, Risk Assessment, Toxicity Tests, Endocrine disrupting chemicals, Systematic review, Study evaluation, Strength of evidence, Weight of evidence, Adverse effect, Endocrine disrupting activity, Evidence integration, In vivo, Public Health and Health Services, Toxicology, Public health
Abstract

BackgroundThe issue of endocrine disrupting chemicals (EDCs) is receiving wide attention from both the scientific and regulatory communities. Recent analyses of the EDC literature have been criticized for failing to use transparent and objective approaches to draw conclusions about the strength of evidence linking EDC exposures to adverse health or environmental outcomes. Systematic review methodologies are ideal for addressing this issue as they provide transparent and consistent approaches to study selection and evaluation. Objective methods are needed for integrating the multiple streams of evidence (epidemiology, wildlife, laboratory animal, in vitro, and in silico data) that are relevant in assessing EDCs.MethodsWe have developed a framework for the systematic review and integrated assessment (SYRINA) of EDC studies. The framework was designed for use with the International Program on Chemical Safety (IPCS) and World Health Organization (WHO) definition of an EDC, which requires appraisal of evidence regarding 1) association between exposure and an adverse effect, 2) association between exposure and endocrine disrupting activity, and 3) a plausible link between the adverse effect and the endocrine disrupting activity.ResultsBuilding from existing methodologies for evaluating and synthesizing evidence, the SYRINA framework includes seven steps: 1) Formulate the problem; 2) Develop the review protocol; 3) Identify relevant evidence; 4) Evaluate evidence from individual studies; 5) Summarize and evaluate each stream of evidence; 6) Integrate evidence across all streams; 7) Draw conclusions, make recommendations, and evaluate uncertainties. The proposed method is tailored to the IPCS/WHO definition of an EDC but offers flexibility for use in the context of other definitions of EDCs.ConclusionsWhen using the SYRINA framework, the overall objective is to provide the evidence base needed to support decision making, including any action to avoid/minimise potential adverse effects of exposures. This framework allows for the evaluation and synthesis of evidence from multiple evidence streams. Finally, a decision regarding regulatory action is not only dependent on the strength of evidence, but also the consequences of action/inaction, e.g. limited or weak evidence may be sufficient to justify action if consequences are serious or irreversible.

Published
2016

13. Out of REACH : environmental hazards of cosmetic preservatives

Author

Kättström, Diana, Beronius, Anna, af Gennas, Urban Boije, Rudén, Christina, Ågerstrand, Marlene, Kättström, Diana, Beronius, Anna, af Gennas, Urban Boije, Rudén, Christina, and Ågerstrand, Marlene

Abstract

The EU Cosmetic Products Regulation requires neither environmental data nor environmental risk assessment for individual ingredients or finished cosmetic products. Instead, it relies on REACH to address environmental risks linked to cosmetic ingredients, including preservatives. We investigated how the environmental risks of cosmetic preservatives are managed by REACH. We identified preservatives of environmental concern and examined if any of these had been selected for Substance Evaluation, proposed for or identified as an SVHC, required authorization or were proposed for, or subject to, restriction under REACH. More than half of the preservatives approved under the Cosmetic Product Regulation, 70 of 137, were identified as being of environmental concern according to the criteria set in this study. Some of the approved preservatives were no longer produced or used in the EU due to their hazardous properties. However, they remained approved and may still enter the EU via the imported products. Our results also indicate that the environmental aspects of cosmetic ingredients, including preservatives, are not efficiently managed by REACH. Besides the known issues in REACH, we identified additional areas in the interface between REACH, CLP and the Cosmetic Products Regulation that call for improvement. Here, we provide practical suggestions in line with the Chemicals Strategy for Sustainability. If implemented, these measures would strengthen the protection of the environment from hazardous cosmetic ingredients.

Published
2024
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14. Applying a modified systematic review and integrated assessment framework (SYRINA) – a case study on triphenyl phosphate †

Author

Bui, Thuy T., Aasa, Jenny, Abass, Khaled, Ågerstrand, Marlene, Beronius, Anna, Castro, Mafalda, Escrivá, Laura, Galizia, Audrey, Gliga, Anda, Karlsson, Oskar, Whaley, Paul, Yost, Erin, Rudén, Christina, Bui, Thuy T., Aasa, Jenny, Abass, Khaled, Ågerstrand, Marlene, Beronius, Anna, Castro, Mafalda, Escrivá, Laura, Galizia, Audrey, Gliga, Anda, Karlsson, Oskar, Whaley, Paul, Yost, Erin, and Rudén, Christina

Abstract

This work presents a case study in applying a systematic review framework (SYRINA) to the identification of chemicals as endocrine disruptors. The suitability and performance of the framework is tested with regard to the widely accepted World Health Organization definition of an endocrine disruptor (ED). The endocrine disrupting potential of triphenyl phosphate (TPP), a well-studied flame retardant reported to exhibit various endocrine related effects was assessed. We followed the 7 steps of the SYRINA framework, articulating the research objective via Populations, Exposures, Comparators, Outcomes (PECO) statements, performed literature search and screening, conducted study evaluation, performed data extraction and summarized and integrated the evidence. Overall, 66 studies, consisting of in vivo, in vitro and epidemiological data, were included. We concluded that triphenyl phosphate could be identified as an ED based on metabolic disruption and reproductive function. We found that the tools used in this case study and the optimizations performed on the framework were suitable to assess properties of EDs. A number of challenges and areas for methodological development in systematic appraisal of evidence relating to endocrine disrupting potential were identified; significant time and effort were needed for the analysis of in vitro mechanistic data in this case study, thus increasing the workload and time needed to perform the systematic review process. Further research and development of this framework with regards to grey literature (non-peer-reviewed literature) search, harmonization of study evaluation methods, more consistent evidence integration approaches and a pre-defined method to assess links between adverse effect and endocrine activity are recommended. It would also be advantageous to conduct more case studies for a chemical with less data than TPP.

Published
2024

15. Applying a modified systematic review and integrated assessment framework (SYRINA) - a case study on triphenyl phosphate

Author

Bui, Thuy T, Aasa, Jenny, Abass, Khaled, Ågerstrand, Marlene, Beronius, Anna, Castro, Mafalda, Escrivá, Laura, Galizia, Audrey, Gliga, Anda, Karlsson, Oskar, Whaley, Paul, Yost, Erin, Rudén, Christina, Bui, Thuy T, Aasa, Jenny, Abass, Khaled, Ågerstrand, Marlene, Beronius, Anna, Castro, Mafalda, Escrivá, Laura, Galizia, Audrey, Gliga, Anda, Karlsson, Oskar, Whaley, Paul, Yost, Erin, and Rudén, Christina

Abstract

This work presents a case study in applying a systematic review framework (SYRINA) to the identification of chemicals as endocrine disruptors. The suitability and performance of the framework is tested with regard to the widely accepted World Health Organization definition of an endocrine disruptor (ED). The endocrine disrupting potential of triphenyl phosphate (TPP), a well-studied flame retardant reported to exhibit various endocrine related effects was assessed. We followed the 7 steps of the SYRINA framework, articulating the research objective via Populations, Exposures, Comparators, Outcomes (PECO) statements, performed literature search and screening, conducted study evaluation, performed data extraction and summarized and integrated the evidence. Overall, 66 studies, consisting of in vivo, in vitro and epidemiological data, were included. We concluded that triphenyl phosphate could be identified as an ED based on metabolic disruption and reproductive function. We found that the tools used in this case study and the optimizations performed on the framework were suitable to assess properties of EDs. A number of challenges and areas for methodological development in systematic appraisal of evidence relating to endocrine disrupting potential were identified; significant time and effort were needed for the analysis of in vitro mechanistic data in this case study, thus increasing the workload and time needed to perform the systematic review process. Further research and development of this framework with regards to grey literature (non-peer-reviewed literature) search, harmonization of study evaluation methods, more consistent evidence integration approaches and a pre-defined method to assess links between adverse effect and endocrine activity are recommended. It would also be advantageous to conduct more case studies for a chemical with less data than TPP., This work presents a case study in applying a systematic review framework (SYRINA) to the identification of chemicals as endocrine disruptors. The suitability and performance of the framework is tested with regard to the widely accepted World Health Organization definition of an endocrine disruptor (ED). The endocrine disrupting potential of triphenyl phosphate (TPP), a well-studied flame retardant reported to exhibit various endocrine related effects was assessed. We followed the 7 steps of the SYRINA framework, articulating the research objective via Populations, Exposures, Comparators, Outcomes (PECO) statements, performed literature search and screening, conducted study evaluation, performed data extraction and summarized and integrated the evidence. Overall, 66 studies, consisting of in vivo, in vitro and epidemiological data, were included. We concluded that triphenyl phosphate could be identified as an ED based on metabolic disruption and reproductive function. We found that the tools used in this case study and the optimizations performed on the framework were suitable to assess properties of EDs. A number of challenges and areas for methodological development in systematic appraisal of evidence relating to endocrine disrupting potential were identified; significant time and effort were needed for the analysis of in vitro mechanistic data in this case study, thus increasing the workload and time needed to perform the systematic review process. Further research and development of this framework with regards to grey literature (non-peer-reviewed literature) search, harmonization of study evaluation methods, more consistent evidence integration approaches and a pre-defined method to assess links between adverse effect and endocrine activity are recommended. It would also be advantageous to conduct more case studies for a chemical with less data than TPP.

Published
2024

16. Building an adverse outcome pathway network for estrogen-, androgen- and steroidogenesis-mediated reproductive toxicity

Author

Zilliacus, Johanna, Draskau, Monica K., Johansson, Hanna K. L., Svingen, Terje, Beronius, Anna, Zilliacus, Johanna, Draskau, Monica K., Johansson, Hanna K. L., Svingen, Terje, and Beronius, Anna

Abstract

Introduction: Adverse Outcome Pathways (AOPs) can support both testing and assessment of endocrine disruptors (EDs). There is, however, a need for further development of the AOP framework to improve its applicability in a regulatory context. Here we have inventoried the AOP-wiki to identify all existing AOPs related to mammalian reproductive toxicity arising from disruption to the estrogen, androgen, and steroidogenesis modalities. Core key events (KEs) shared between relevant AOPs were also identified to aid in further AOP network (AOPN) development. Methods: A systematic approach using two different methods was applied to screen and search the entire AOP-wiki library. An AOPN was visualized using Cytoscape. Manual refinement was performed to remove AOPS devoid of any KEs and/or KERs. Results: Fifty-eight AOPs relevant for mammalian reproductive toxicity were originally identified, with 42 AOPs included in the final AOPN. Several of the KEs and KE relationships (KERs) described similar events and were thus merged to optimize AOPN construction. Sixteen sub-networks related to effects on hormone levels or hormone activity, cancer outcomes, male and female reproductive systems, and overall effects on fertility and reproduction were identified within the AOPN. Twenty-six KEs and 11 KERs were identified as core blocks of knowledge in the AOPN, of which 19 core KEs are already included as parameters in current OECD and US EPA test guidelines. Discussion: The AOPN highlights knowledge gaps that can be targeted for further development of a more complete AOPN that can support the identification and assessment of EDs.

Published
2024

17. Recommendations for the conduct of systematic reviews in toxicology and environmental health research (COSTER)

Author

Whaley, Paul, Aiassa, Elisa, Beausoleil, Claire, Beronius, Anna, Bilotta, Gary, Boobis, Alan, de Vries, Rob, Hanberg, Annika, Hoffmann, Sebastian, Hunt, Neil, Kwiatkowski, Carol F., Lam, Juleen, Lipworth, Steven, Martin, Olwenn, Randall, Nicola, Rhomberg, Lorenz, Rooney, Andrew A., Schünemann, Holger J., Wikoff, Daniele, Wolffe, Taylor, and Halsall, Crispin

Published
2020
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19. Applying a modified systematic review and integrated assessment framework (SYRINA) – A case study on Triphenyl Phosphate

Author

Bui, Thuy, primary, Aasa, Jenny, additional, Abass, Khaled, additional, Ågerstrand, Marlene, additional, Beronius, Anna Sofia, additional, Castro, Mafalda, additional, Escrivá, Laura, additional, Galizia, Audrey, additional, Gliga, Anda R., additional, Karlsson, Oskar, additional, Whaley, Paul, additional, Yost, Erin, additional, and Rudén, Christina, additional

Published
2024
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20. Protocol: Testing the Performance of INVITES-IN, A Tool for Assessing the Internal Validity of In Vitro Studies

Author

Mathisen, Gro H., primary, Vist, Gunn E., additional, Whaley, Paul, additional, White, Richard A., additional, Husøy, Trine, additional, Ames, Heather M., additional, Beronius, Anna, additional, Di Consiglio, Emma, additional, Druwe, Ingrid, additional, Hartung, Thomas, additional, Hoffmann, Sebastian, additional, Hooijmans, Carlijn R., additional, Machera, Kyriaki, additional, Prieto, Pilar, additional, Robinson, Joshua F., additional, Roggen, Erwin, additional, Rooney, Andrew A., additional, Roth, Nicolas, additional, Spilioti, Eliana, additional, Spyropoulou, Anastasia, additional, Tcheremenskaia, Olga, additional, Testai, Emanuela, additional, Vinken, Mathieu, additional, and Svendsen, Camilla, additional

Published
2023
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22. Beyond Chemicals: Opportunities and Challenges of Integrating Non-chemical Stressors in Adverse Outcome Pathways.

Author

Clerbaux, Laure-Alix, Filipovska, Julija, Nymark, Penny, Chauhan, Vinita, Sewald, Katherina, Alb, Miriam, Sachana, Madgalini, Beronius, Anna, Amorim, Maria-Joao, and Wittwehr, Clemens

Abstract

Adverse outcome pathways (AOPs) were developed to accelerate evidence-based chemical risk assessment by leveraging data from new approach methodologies. Thanks to their stressor-agnostic approach, AOPs were seen as instrumental in other fields. Here, we present AOPs that report non-chemical stressors along with the challenges encountered for their development. Challenges regarding AOPs linked to nanomaterials include non-specific molecular initiating events, limited understanding of nanomaterial biodistribution, and needs for adaptations of in silico modeling and testing systems. Development of AOPs for radiation faces challenges in how to incorporate ionizing events type, dose rate, energy deposition, and how to account for targeting multiple macromolecules. AOPs for COVID-19 required the inclusion of SARS-CoV-2-specific replicative steps to capture the essential events driving the disease. Developing AOPs to evaluate efficacy and toxicity of cell therapies necessitates addressing the cellular nature and the therapeutic function of the stressor. Finally, addressing toxicity of emerging biological stressors like microbial pesticides can learn from COVID-19 AOPs. We further discuss that the adaptations needed to expand AOP applicability beyond chemicals are mainly at the molecular and cellular levels, while downstream key events at tissue or organ level, such as inflammation, are shared by many AOPs initiated by various stressors. In conclusion, although it is challenging to integrate non-chemical stressors within AOPs, this expands opportunities to account for real-world scenarios, to identify vulnerable individuals, and to bridge knowledge on mechanisms of adversity. [ABSTRACT FROM AUTHOR]

Published
2024
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24. Protocol for designing INVITES-IN, a tool for assessing the internal validity of in vitro studies

Author

Svendsen, Camilla, primary, Whaley, Paul, additional, Vist, Gunn E., additional, Husøy, Trine, additional, Beronius, Anna, additional, Di Consiglio, Emma, additional, Druwe, Ingrid, additional, Hartung, Thomas, additional, Hatzi, Vasiliki I., additional, Hoffmann, Sebastian, additional, Hooijmans, Carlijn R., additional, Machera, Kyriaki, additional, Robinson, Joshua F., additional, Roggen, Erwin, additional, Rooney, Andrew A., additional, Roth, Nicolas, additional, Spilioti, Eliana, additional, Spyropoulou, Anastasia, additional, Tcheremenskaia, Olga, additional, Testai, Emanuela, additional, Vinken, Mathieu, additional, and Mathisen, Gro H., additional

Published
2023
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26. Applying a modified systematic review and integrated assessment framework (SYRINA) - a case study on triphenyl phosphate

Author

Bui, Thuy T., Aasa, Jenny, Abass, Khaled, Ågerstrand, Marlene, Beronius, Anna, Castro, Mafalda, Escrivá, Laura, Galizia, Audrey, Gliga, Anda, Karlsson, Oskar, Whaley, Paul, Yost, Erin, Rudén, Christina, Bui, Thuy T., Aasa, Jenny, Abass, Khaled, Ågerstrand, Marlene, Beronius, Anna, Castro, Mafalda, Escrivá, Laura, Galizia, Audrey, Gliga, Anda, Karlsson, Oskar, Whaley, Paul, Yost, Erin, and Rudén, Christina

Abstract

This work presents a case study in applying a systematic review framework (SYRINA) to the identification of chemicals as endocrine disruptors. The suitability and performance of the framework is tested with regard to the widely accepted World Health Organization definition of an endocrine disruptor (ED). The endocrine disrupting potential of triphenyl phosphate (TPP), a well-studied flame retardant reported to exhibit various endocrine related effects was assessed. We followed the 7 steps of the SYRINA framework, articulating the research objective via Populations, Exposures, Comparators, Outcomes (PECO) statements, performed literature search and screening, conducted study evaluation, performed data extraction and summarized and integrated the evidence. Overall, 66 studies, consisting of in vivo, in vitro and epidemiological data, were included. We concluded that triphenyl phosphate could be identified as an ED based on metabolic disruption and reproductive function. We found that the tools used in this case study and the optimizations performed on the framework were suitable to assess properties of EDs. A number of challenges and areas for methodological development in systematic appraisal of evidence relating to endocrine disrupting potential were identified; significant time and effort were needed for the analysis of in vitro mechanistic data in this case study, thus increasing the workload and time needed to perform the systematic review process. Further research and development of this framework with regards to grey literature (non-peer-reviewed literature) search, harmonization of study evaluation methods, more consistent evidence integration approaches and a pre-defined method to assess links between adverse effect and endocrine activity are recommended. It would also be advantageous to conduct more case studies for a chemical with less data than TPP.

Published
2023
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27. Protocol: Testing the Performance of INVITES-IN, A Tool for Assessing the Internal Validity of In Vitro Studies

Author

Mathisen, Gro H., Vist, Gunn E., Whaley, Paul, White, Richard A., Husøy, Trine, Ames, Heather M., Beronius, Anna, Di Consiglio, Emma, Druwe, Ingrid, Hartung, Thomas, Hoffmann, Sebastian, Hooijmans, Carlijn R., Machera, Kyriaki, Prieto, Pilar, Robinson, Joshua F., Roggen, Erwin, Rooney, Andrew A., Roth, Nicolas, Spilioti, Eliana, Spyropoulou, Anastasia, Tcheremenskaia, Olga, Testai, Emanuela, Vinken, Mathieu, Svendsen, Camilla, Mathisen, Gro H., Vist, Gunn E., Whaley, Paul, White, Richard A., Husøy, Trine, Ames, Heather M., Beronius, Anna, Di Consiglio, Emma, Druwe, Ingrid, Hartung, Thomas, Hoffmann, Sebastian, Hooijmans, Carlijn R., Machera, Kyriaki, Prieto, Pilar, Robinson, Joshua F., Roggen, Erwin, Rooney, Andrew A., Roth, Nicolas, Spilioti, Eliana, Spyropoulou, Anastasia, Tcheremenskaia, Olga, Testai, Emanuela, Vinken, Mathieu, and Svendsen, Camilla

Published
2023

28. Protocol for designing INVITES-IN, a tool for assessing the internal validity of in vitro studies

Author

Svendsen, Camilla, Whaley, Paul, Vist, Gunn E., Husøy, Trine, Beronius, Anna, Di Consiglio, Emma, Druwe, Ingrid, Hartung, Thomas, Hatzi, Vasiliki I., Hoffmann, Sebastian, Hooijmans, Carlijn R., Machera, Kyriaki, Robinson, Joshua F., Roggen, Erwin, Rooney, Andrew A., Roth, Nicolas, Spilioti, Eliana, Spyropoulou, Anastasia, Tcheremenskaia, Olga, Testai, Emanuela, Vinken, Mathieu, Mathisen, Gro H., Svendsen, Camilla, Whaley, Paul, Vist, Gunn E., Husøy, Trine, Beronius, Anna, Di Consiglio, Emma, Druwe, Ingrid, Hartung, Thomas, Hatzi, Vasiliki I., Hoffmann, Sebastian, Hooijmans, Carlijn R., Machera, Kyriaki, Robinson, Joshua F., Roggen, Erwin, Rooney, Andrew A., Roth, Nicolas, Spilioti, Eliana, Spyropoulou, Anastasia, Tcheremenskaia, Olga, Testai, Emanuela, Vinken, Mathieu, and Mathisen, Gro H.

Abstract

This protocol describes the design and development of a tool for evaluation of the internal validity of in vitro studies, which is needed to include the data as evidence in systematic reviews and chemical risk assessments. The tool will be designed specifically to be applied to cell culture studies, including, but not restricted to, studies meeting the new approach methodology (NAM) definition. The tool is called INVITES-IN (IN VITro Experimental Studies INternal validity). In this protocol, three of the four studies that will be performed to create the release version of INVITES-IN are described. In the first study, evaluation of existing assessment tools will be combined with focus group discussions to identify how characteristics of the design or conduct of an in vitro study can affect its internal validity. Bias domains and items considered to be of relevance for in vitro studies will be identified. In the second study, group agreement on internal validity domains and items of importance for in vitro studies will be identified via a modified Delphi methodology. In the third study, the draft version of the tool will be created, based on the data on relevance and importance of bias domains and items collected in Studies 1 and 2. A separate protocol will be prepared for the fourth study, which includes the user testing and validation of the tool, and collection of users’ experience.

Published
2023

30. Application of AOPs to assist regulatory assessment of chemical risks – Case studies, needs and recommendations

Author

Bajard, Lola, primary, Adamovsky, Ondrej, additional, Audouze, Karine, additional, Baken, Kirsten, additional, Barouki, Robert, additional, Beltman, Joost B., additional, Beronius, Anna, additional, Bonefeld-Jørgensen, Eva Cecilie, additional, Cano-Sancho, German, additional, de Baat, Milo L., additional, Di Tillio, Filippo, additional, Fernández, Mariana F., additional, FitzGerald, Rex E., additional, Gundacker, Claudia, additional, Hernández, Antonio F., additional, Hilscherova, Klara, additional, Karakitsios, Spyros, additional, Kuchovska, Eliska, additional, Long, Manhai, additional, Luijten, Mirjam, additional, Majid, Sanah, additional, Marx-Stoelting, Philip, additional, Mustieles, Vicente, additional, Negi, Chander K., additional, Sarigiannis, Dimosthenis, additional, Scholz, Stefan, additional, Sovadinova, Iva, additional, Stierum, Rob, additional, Tanabe, Shihori, additional, Tollefsen, Knut Erik, additional, van den Brand, Annick D., additional, Vogs, Carolina, additional, Wielsøe, Maria, additional, Wittwehr, Clemens, additional, and Blaha, Ludek, additional

Published
2023
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31. Application of AOPs to assist regulatory assessment of chemical risks - Case studies, needs and recommendations

Author

Bajard, Lola, Adamovsky, Ondrej, Audouze, Karine, Baken, Kirsten, Barouki, Robert, Beltman, Joost B., Beronius, Anna, Bonefeld-Jorgensen, Eva Cecilie, Cano-Sancho, German, de Baat, Milo L., Di Tillio, Filippo, Fernandez, Mariana F., FitzGerald, Rex E., Gundacker, Claudia, Hernandez, Antonio F., Hilscherova, Klara, Karakitsios, Spyros, Kuchovska, Eliska, Long, Manhai, Luijten, Mirjam, Majid, Sanah, Marx-Stoelting, Philip, Mustieles, Vicent, Negi, Chander K., Sarigiannis, Dimosthenis, Scholz, Stefan, Sovadinova, Iva, Stierum, Rob, Tanabe, Shihori, Tollefsen, Knut Erik, van den Brand, Annick D., Vogs, Carolina, Wielsoe, Maria, Wittwehr, Clemens, and Blaha, Ludek

Subjects
Public Health, Global Health, Social Medicine and Epidemiology
Abstract

While human regulatory risk assessment (RA) still largely relies on animal studies, new approach methodologies (NAMs) based on in vitro, in silico or non-mammalian alternative models are increasingly used to evaluate chemical hazards. Moreover, human epidemiological studies with biomarkers of effect (BoE) also play an invaluable role in identifying health effects associated with chemical exposures. To move towards the next generation risk assessment (NGRA), it is therefore crucial to establish bridges between NAMs and standard approaches, and to establish processes for increasing mechanistically-based biological plausibility in human studies. The Adverse Outcome Pathway (AOP) framework constitutes an important tool to address these needs but, despite a significant increase in knowledge and awareness, the use of AOPs in chemical RA remains limited. The objective of this paper is to address issues related to using AOPs in a regulatory context from various perspectives as it was discussed in a workshop organized within the European Union partnerships HBM4EU and PARC in spring 2022. The paper presents examples where the AOP framework has been proven useful for the human RA process, particularly in hazard prioritization and characterization, in integrated approaches to testing and assessment (IATA), and in the identification and validation of BoE in epidemiological studies. Nevertheless, several limitations were identified that hinder the optimal usability and acceptance of AOPs by the regulatory community including the lack of quantitative information on response-response relationships and of efficient ways to map chemical data (exposure and toxicity) onto AOPs. The paper summarizes suggestions, ongoing initiatives and third-party tools that may help to overcome these obstacles and thus assure better implementation of AOPs in the NGRA.

Published
2023

34. Factors Modulating COVID-19 : A Mechanistic Understanding Based on the Adverse Outcome Pathway Framework

Author

Clerbaux, Laure Alix, Albertini, Maria Cristina, Amigó, Núria, Beronius, Anna, Bezemer, Gillina F.G., Coecke, Sandra, Daskalopoulos, Evangelos P., del Giudice, Giusy, Greco, Dario, Grenga, Lucia, Mantovani, Alberto, Muñoz, Amalia, Omeragic, Elma, Parissis, Nikolaos, Petrillo, Mauro, Saarimäki, Laura A., Soares, Helena, Sullivan, Kristie, Landesmann, Brigitte, Tampere University, and BioMediTech

Subjects
3111 Biomedicine
Abstract

Addressing factors modulating COVID-19 is crucial since abundant clinical evidence shows that outcomes are markedly heterogeneous between patients. This requires identifying the factors and understanding how they mechanistically influence COVID-19. Here, we describe how eleven selected factors (age, sex, genetic factors, lipid disorders, heart failure, gut dysbiosis, diet, vitamin D deficiency, air pollution and exposure to chemicals) influence COVID-19 by applying the Adverse Outcome Pathway (AOP), which is well-established in regulatory toxicology. This framework aims to model the sequence of events leading to an adverse health outcome. Several linear AOPs depicting pathways from the binding of the virus to ACE2 up to clinical outcomes observed in COVID-19 have been developed and integrated into a network offering a unique overview of the mechanisms underlying the disease. As SARS-CoV-2 infectibility and ACE2 activity are the major starting points and inflammatory response is central in the development of COVID-19, we evaluated how those eleven intrinsic and extrinsic factors modulate those processes impacting clinical outcomes. Applying this AOP-aligned approach enables the identification of current knowledge gaps orientating for further research and allows to propose biomarkers to identify of high-risk patients. This approach also facilitates expertise synergy from different disciplines to address public health issues. publishedVersion

Published
2022

35. Factors Modulating COVID-19

Author

Clerbaux, Laure Alix, Albertini, Maria Cristina, Amigó, Núria, Beronius, Anna, Bezemer, Gillina F.G., Coecke, Sandra, Daskalopoulos, Evangelos P., del Giudice, Giusy, Greco, Dario, Grenga, Lucia, Mantovani, Alberto, Muñoz, Amalia, Omeragic, Elma, Parissis, Nikolaos, Petrillo, Mauro, Saarimäki, Laura A., Soares, Helena, Sullivan, Kristie, Landesmann, Brigitte, NOVA Medical School|Faculdade de Ciências Médicas (NMS|FCM), and Centro de Estudos de Doenças Crónicas (CEDOC)

Subjects
Medicine(all), co-morbidities, lifestyle, age, SDG 3 - Good Health and Well-being, SARS-CoV-2 infection, COVID-19, sex, pre-existing conditions, environment, adverse outcome pathway, modulating factors
Abstract

Funding Information: The work was performed under the JRC Exploratory Research project CIAO—Modelling COVID-19 pathogenesis using the Adverse Outcome Pathway (AOP). Julija Filipovska for her careful reading and valuable inputs. Funding: This research was funded by the Academy of Finland (grand number 322761) for D.G., G.d.G. and L.A.S. and by Fundação para a Ciência e Tecnologia through CEECIND/01049/2020 for H.S. For the other authors, this research received no external funding. Addressing factors modulating COVID-19 is crucial since abundant clinical evidence shows that outcomes are markedly heterogeneous between patients. This requires identifying the factors and understanding how they mechanistically influence COVID-19. Here, we describe how eleven selected factors (age, sex, genetic factors, lipid disorders, heart failure, gut dysbiosis, diet, vitamin D deficiency, air pollution and exposure to chemicals) influence COVID-19 by applying the Adverse Outcome Pathway (AOP), which is well-established in regulatory toxicology. This framework aims to model the sequence of events leading to an adverse health outcome. Several linear AOPs depicting pathways from the binding of the virus to ACE2 up to clinical outcomes observed in COVID-19 have been developed and integrated into a network offering a unique overview of the mechanisms underlying the disease. As SARS-CoV-2 infectibility and ACE2 activity are the major starting points and inflammatory response is central in the development of COVID-19, we evaluated how those eleven intrinsic and extrinsic factors modulate those processes impacting clinical outcomes. Applying this AOP-aligned approach enables the identification of current knowledge gaps orientating for further research and allows to propose biomarkers to identify of high-risk patients. This approach also facilitates expertise synergy from different disciplines to address public health issues. publishersversion published

Published
2022

37. Factors Modulating COVID-19: A Mechanistic Understanding Based on the Adverse Outcome Pathway Framework

Author

Clerbaux, Laure-Alix, primary, Albertini, Maria Cristina, additional, Amigó, Núria, additional, Beronius, Anna, additional, Bezemer, Gillina F. G., additional, Coecke, Sandra, additional, Daskalopoulos, Evangelos P., additional, del Giudice, Giusy, additional, Greco, Dario, additional, Grenga, Lucia, additional, Mantovani, Alberto, additional, Muñoz, Amalia, additional, Omeragic, Elma, additional, Parissis, Nikolaos, additional, Petrillo, Mauro, additional, Saarimäki, Laura A., additional, Soares, Helena, additional, Sullivan, Kristie, additional, and Landesmann, Brigitte, additional

Published
2022
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40. Evaluation of EFSA training courses on principles in chemical and biological risk assessment

Author

Escher, Sylvia, Bruer, Gustav, Creutzenberg, Otto, Schlemminger, Karin, Schulz, Florian, Ziemann, Christina, Rorije, Emiel, Klaveren, Jacob van, Posthuma, Leo, Bokkers, Bas, Slob, Wout, Hanberg, Annika, Beronius, Anna, Baumann, Lisa, Zilliacus, Johanna, Bitsch, Annette, and Publica

Abstract

This report evaluates the training courses delivered under the contract OC/EFSA/SCER/2017/01 ‐ Lot 1. Within the period of January 2018 to February 2022 a total of 21 training courses were provided, eight on‐site training courses in Parma at EFSA, six virtual training courses during the Covid‐19 pandemic and seven eLearning courses comprising various numbers of modules. The courses covered different aspects of chemical and biological risk assessment and related tools, namely i) harmonisation of risk assessment methodologies for human health and ecological risk assessment of combined exposure to multiple chemicals (mixture assessment), ii) risk assessment of the application of nanoscience and nanotechnologies in agro/food/feed (nanotoxicity); iii) science‐based criteria for identifying endocrine disruptors in the context of EU legislation on pesticides and biocides (endocrine disruption); iv) principles on genotoxicity on scientific assessment (genotoxicity) and v) computational toxicology approaches and tools (in silico). All tutors were experts in their field and had previously performed training courses on these topics. The target participants of the training courses were members of EFSA’s Scientific Committee/Panels and their working groups as well as employees from national and international regulatory agencies associated with risk assessment of feed and food compounds. Members of the EFSA Networks as well as EFSA scientific staff also participated in the training courses. Courses were evaluated based on the feedback of participants and continuously improved also by integrating updated or new EFSA guidance documents.

Published
2022

41. COVID-19 through adverse outcome pathways: building networks to better understand the disease: report of the 3rd CIAO AOP design workshop

Author

Clerbaux, Laure-Alix, Amigó, Núria, Amorim, Maria João, Bal-Price, Anna, Leite, Sofia Batista, Beronius, Anna, Bezemer, Gillina F.G., Bostroem, Ann-Charlotte, Carusi, Annamaria, Coecke, Sandra, Concha, Rachel, Daskalopoulos, Evangelos P., Debernardi, Francesca, Edrosa, Eizleayne, Edwards, Steve W., Filipovska, Julija, Garcia-Reyero, Natàlia, Gavins, Felicity N.E., Halappanavar, Sabina, Hargreaves, Alan J., Hogberg, Helena, Huynh, Mylène T., Jacobson, Daniel, Josephs-Spaulding, Jonathan, Kim, Young Jun, Kong, Hyun Joon, Krebs, Catharine E., Lam, Ann, Landesmann, Brigitte, Racanelli Layton, Adrienne, Lee, Yong Oh, Macmillan, Donna S., Mantovani, Alberto, Margiotta-Casaluci, Luigi, Martens, Marvin, Masereeuw, Rosalinde, Mayasich, Sally A., Mei, Liang Merlin, Mortensen, Holly, Munoz Pineiro, Amalia, Nymark, Penny, Ohayon, Elan, Manoj Ojasi, Joshi, Paini, Alicia, Parissis, Nikolaos, Parvatam, Surat, Pistollato, Francesca, Sachana, Magdalini, Birkelund Sørli, Jorid, Sullivan, Kristie M., Sund, Jukka, Tanabe, Shihori, Tsaioun, Katya, Vinken, Mathieu, Viviani, Laura, Waspe, Jennifer, Willett, Catherine, Wittwehr, Clemens, Pharmaceutical and Pharmacological Sciences, and Experimental in vitro toxicology and dermato-cosmetology

Abstract

On April 28-29, 2021, 50 scientists from different fields of expertise met for the 3rd online CIAO workshop. The CIAO project “Modelling the Pathogenesis of COVID-19 using the Adverse Outcome Pathway (AOP) framework” aims at building a holistic assembly of the available scientific knowledge on COVID-19 using the AOP framework. An individual AOP depicts the disease progression from the initial contact with the SARS-CoV-2 virus through biological key events (KE) toward an adverse outcome such as respiratory distress, anosmia or multiorgan failure. Assembling the individual AOPs into a network highlights shared KEs as central biological nodes involved in multiple outcomes observed in COVID-19 patients. During the workshop, the KEs and AOPs established so far by the CIAO members were presented and posi­tioned on a timeline of the disease course. Modulating factors influencing the progression and severity of the disease were also addressed as well as factors beyond purely biological phenomena. CIAO relies on an interdisciplinary crowd­sourcing effort, therefore, approaches to expand the CIAO network by widening the crowd and reaching stakeholders were also discussed. To conclude the workshop, it was decided that the AOPs/KEs will be further consolidated, inte­grating virus variants and long COVID when relevant, while an outreach campaign will be launched to broaden the CIAO scientific crowd.

Published
2022

42. COVID-19 through Adverse Outcome Pathways: Building networks to better understand the disease - 3rd CIAO AOP Design Workshop

Author

Clerbaux, Laure-Alix, Amigó, Núria, Amorim, Maria João, Bal-Price, Anna, Batista Leite, Sofia, Beronius, Anna, Bostroem, Ann-Charlotte, Carusi, Annamaria, Coecke, Sandra, Concha, Rachel, Daskalopoulos, Evangelos P, Debernardi, Francesca, Edrosa, Eizleayne, Edwards, Steve W, Filipovska, Julija, Garcia-Reyero, Natàlia, Gavins, Felicity N E, Halappanavar, Sabina, Hargreaves, Alan J, Hogberg, Helena T, Huynh, Mylène T, Jacobson, Daniel, Josephs-Spaulding, Jonathan, Kim, Young Jun, Kong, Hyun Joon, Krebs, Catharine E, Lam, Ann, Landesmann, Brigitte, Layton, Adrienne, Lee, Yong Oh, Macmillan, Donna S, Mantovani, Alberto, Margiotta-Casaluci, Luigi, Martens, Marvin, Masereeuw, Rosalinde, Mayasich, Sally A, Mei, Liang Merlin, Mortensen, Holly, Munoz Pineiro, Amalia, Nymark, Penny, Ohayon, Elan, Ojasi, Joshi, Paini, Alicia, Parissis, Nikolaos, Parvatam, Surat, Pistollato, Francesca, Sachana, Magdalini, Sørli, Jorid Birkelund, Sullivan, Kristie M, Sund, Jukka, Tanabe, Shihori, Tsaioun, Katya, Vinken, Mathieu, Viviani, Laura, Waspe, Jennifer, Willett, Catherine, Wittwehr, Clemens, Clerbaux, Laure-Alix, Amigó, Núria, Amorim, Maria João, Bal-Price, Anna, Batista Leite, Sofia, Beronius, Anna, Bostroem, Ann-Charlotte, Carusi, Annamaria, Coecke, Sandra, Concha, Rachel, Daskalopoulos, Evangelos P, Debernardi, Francesca, Edrosa, Eizleayne, Edwards, Steve W, Filipovska, Julija, Garcia-Reyero, Natàlia, Gavins, Felicity N E, Halappanavar, Sabina, Hargreaves, Alan J, Hogberg, Helena T, Huynh, Mylène T, Jacobson, Daniel, Josephs-Spaulding, Jonathan, Kim, Young Jun, Kong, Hyun Joon, Krebs, Catharine E, Lam, Ann, Landesmann, Brigitte, Layton, Adrienne, Lee, Yong Oh, Macmillan, Donna S, Mantovani, Alberto, Margiotta-Casaluci, Luigi, Martens, Marvin, Masereeuw, Rosalinde, Mayasich, Sally A, Mei, Liang Merlin, Mortensen, Holly, Munoz Pineiro, Amalia, Nymark, Penny, Ohayon, Elan, Ojasi, Joshi, Paini, Alicia, Parissis, Nikolaos, Parvatam, Surat, Pistollato, Francesca, Sachana, Magdalini, Sørli, Jorid Birkelund, Sullivan, Kristie M, Sund, Jukka, Tanabe, Shihori, Tsaioun, Katya, Vinken, Mathieu, Viviani, Laura, Waspe, Jennifer, Willett, Catherine, and Wittwehr, Clemens

Abstract

On April 28-29, 2021, 50 scientists from different fields of expertise met for the 3rd online CIAO workshop. The CIAO project “Modelling the Pathogenesis of COVID-19 using the Adverse Outcome Pathway (AOP) framework” aims at building a holistic assembly of the available scientific knowledge on COVID-19 using the AOP framework. An individual AOP depicts the disease progression from the initial contact with the SARS-CoV-2 virus through biological key events (KE) toward an adverse outcome such as respiratory distress, anosmia or multiorgan failure. Assembling the individual AOPs into a network highlights shared KEs as central biological nodes involved in multiple outcomes observed in COVID-19 patients. During the workshop, the KEs and AOPs established so far by the CIAO members were presented and posi­tioned on a timeline of the disease course. Modulating factors influencing the progression and severity of the disease were also addressed as well as factors beyond purely biological phenomena. CIAO relies on an interdisciplinary crowd­sourcing effort, therefore, approaches to expand the CIAO network by widening the crowd and reaching stakeholders were also discussed. To conclude the workshop, it was decided that the AOPs/KEs will be further consolidated, inte­grating virus variants and long COVID when relevant, while an outreach campaign will be launched to broaden the CIAO scientific crowd.

Published
2022

43. COVID-19 through Adverse Outcome Pathways: Building networks to better understand the disease - 3rd CIAO AOP Design Workshop

Author

Afd Pharmacology, Orphan drugs development in The Netherlands: from bench to patient, Pharmacology, Clerbaux, Laure-Alix, Amigó, Núria, Amorim, Maria João, Bal-Price, Anna, Batista Leite, Sofia, Beronius, Anna, Bostroem, Ann-Charlotte, Carusi, Annamaria, Coecke, Sandra, Concha, Rachel, Daskalopoulos, Evangelos P, Debernardi, Francesca, Edrosa, Eizleayne, Edwards, Steve W, Filipovska, Julija, Garcia-Reyero, Natàlia, Gavins, Felicity N E, Halappanavar, Sabina, Hargreaves, Alan J, Hogberg, Helena T, Huynh, Mylène T, Jacobson, Daniel, Josephs-Spaulding, Jonathan, Kim, Young Jun, Kong, Hyun Joon, Krebs, Catharine E, Lam, Ann, Landesmann, Brigitte, Layton, Adrienne, Lee, Yong Oh, Macmillan, Donna S, Mantovani, Alberto, Margiotta-Casaluci, Luigi, Martens, Marvin, Masereeuw, Rosalinde, Mayasich, Sally A, Mei, Liang Merlin, Mortensen, Holly, Munoz Pineiro, Amalia, Nymark, Penny, Ohayon, Elan, Ojasi, Joshi, Paini, Alicia, Parissis, Nikolaos, Parvatam, Surat, Pistollato, Francesca, Sachana, Magdalini, Sørli, Jorid Birkelund, Sullivan, Kristie M, Sund, Jukka, Tanabe, Shihori, Tsaioun, Katya, Vinken, Mathieu, Viviani, Laura, Waspe, Jennifer, Willett, Catherine, Wittwehr, Clemens, Afd Pharmacology, Orphan drugs development in The Netherlands: from bench to patient, Pharmacology, Clerbaux, Laure-Alix, Amigó, Núria, Amorim, Maria João, Bal-Price, Anna, Batista Leite, Sofia, Beronius, Anna, Bostroem, Ann-Charlotte, Carusi, Annamaria, Coecke, Sandra, Concha, Rachel, Daskalopoulos, Evangelos P, Debernardi, Francesca, Edrosa, Eizleayne, Edwards, Steve W, Filipovska, Julija, Garcia-Reyero, Natàlia, Gavins, Felicity N E, Halappanavar, Sabina, Hargreaves, Alan J, Hogberg, Helena T, Huynh, Mylène T, Jacobson, Daniel, Josephs-Spaulding, Jonathan, Kim, Young Jun, Kong, Hyun Joon, Krebs, Catharine E, Lam, Ann, Landesmann, Brigitte, Layton, Adrienne, Lee, Yong Oh, Macmillan, Donna S, Mantovani, Alberto, Margiotta-Casaluci, Luigi, Martens, Marvin, Masereeuw, Rosalinde, Mayasich, Sally A, Mei, Liang Merlin, Mortensen, Holly, Munoz Pineiro, Amalia, Nymark, Penny, Ohayon, Elan, Ojasi, Joshi, Paini, Alicia, Parissis, Nikolaos, Parvatam, Surat, Pistollato, Francesca, Sachana, Magdalini, Sørli, Jorid Birkelund, Sullivan, Kristie M, Sund, Jukka, Tanabe, Shihori, Tsaioun, Katya, Vinken, Mathieu, Viviani, Laura, Waspe, Jennifer, Willett, Catherine, and Wittwehr, Clemens

Published
2022

47. SciRAP workshop report

Author

Beronius, Anna, primary, Ågerstrand, Marlene, additional, Rudén, Christina, additional, and Hanberg, Annika, additional

Published
2017
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48. Additional file 1 of Assessment of the endocrine disrupting properties of bisphenol AF: a case study applying the European regulatory criteria and guidance

Author

Escrivá, Laura, Zilliacus, Johanna, Hessel, Ellen, and Beronius, Anna

Abstract

Additional file 1: Table S1. PECO statements defined for the present study. Table S2. Eligibility criteria stablished for research articles inclusion or exclusion. Table S3: Search terms, data search and number of items retrieved in the BPAF single target search for each database. Table S4: Number of references and date of BPAF search in the three databases and applicants dossier.

Published
2021
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49. Evaluating reliability and risk of bias of in vivo animal data for risk assessment of chemicals - Exploring the use of the SciRAP tool in a systematic review context

Author

Waspe, Jennifer, Bui, Thuy, Dishaw, Laura, Kraft, Andrew, Luke, April, Beronius, Anna, Waspe, Jennifer, Bui, Thuy, Dishaw, Laura, Kraft, Andrew, Luke, April, and Beronius, Anna

Abstract

Within the field of health risk assessment, it is essential that evaluations of reliability or validity of toxicity data are conducted with structure and transparency. To this end, different tools for evaluating toxicity studies have been developed by different groups and organizations, for different specific purposes. The Science in Risk Assessment and Policy (SciRAP) tool was developed for use in the regulatory health risk assessment of chemicals and to promote structured and transparent evaluation of study reliability within European regulatory frameworks. As such, the SciRAP tool is not specifically tailored for use in a systematic review context. However, in light of the current movement towards applying systematic review in the field of environmental health and chemical assessments and European chemicals regulation, we were interested in exploring how SciRAP could be applied in such a context. To achieve this, the scope of the SciRAP tool was first compared to two tools developed based on systematic review principles at the US Environmental Protection Agency's IRIS program and the National Toxicology Program's Office of Health Assessment and Translation (OHAT). Next, the SciRAP and IRIS tools were both applied in a case study to evaluate the same nine in vivo animal studies and the resulting evaluations were compared. The SciRAP tool was found to address the majority of the elements included for study evaluation in the OHAT and IRIS tools. In the case study, no major differences were found in the conclusions drawn when using SciRAP or IRIS tools. However, future developments to bring the SciRAP tool more in line with systematic review principles were identified and are discussed. Overall, this work illustrates the advantages of applying structured and pre-defined methods for study evaluation and provides a unique case study comparing the impact of using different tools for evaluating animal toxicity studies.

Published
2021
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50. A validated search filter for the identification of endocrine disruptors based on the ECHA/EFSA guidance recommendations

Author

Escriva, Laura, Hessel, Ellen, Gustafsson, Susanne, van Spronsen, Rob, Svanberg, Magdalena, Beronius, Anna, Escriva, Laura, Hessel, Ellen, Gustafsson, Susanne, van Spronsen, Rob, Svanberg, Magdalena, and Beronius, Anna

Abstract

A guidance document for the identification of endocrine disruptors (EDs) in the regulatory assessment of plant protection products (PPP) and biocidal products (BP) has been published by the European Chemical Agency (ECHA) and the European Food Safety Authority (EFSA). The ECHA/EFSA guidance, mainly addressing EATS (estrogen, androgen, thyroid, steroidogenesis) modalities, is intended to guide applicants and assessors of the competent regulatory authorities on the implementation of the scientific criteria for the determination of ED properties pursuant to the recently implemented PPP (EU 2018/605) and BP (EU 2017/2100 ) EU Regulations. In this study, a search filter for targeted literature search in context of assessing if a substance can be identified as an ED relevant for human health was developed and validated. Development of the search filter was based on the search strategy presented in the ECHA/EFSA guidance and using the estrogenic chemical Bisphenol AF (BPAF) as a model substance. Information specialists from two independent institutions developed refined search filters based on the suggested original search strategy published (ECHA/EFSA guidance - Appendix F). Articles identified by a systematic literature search for BPAF were screened for relevance with inclusion and exclusion criteria by two independent reviewers obtaining positive (relevant) and negative (irrelevant) controls. The developed search filter was quantitatively evaluated in terms of sensitivity, specificity and precision based on the positive and negative controls. The developed filter was then validated for T modality by its application to the known thyroid-disruptor perchlorate. The result is a sensitive search filter with sufficient specificity, which can be applied for all chemicals where a targeted literature search is needed to assess and identify ED properties of chemicals with relevance for humans. Future application of the filter to a broader range of chemicals may identify further p, QC 20200729

Published
2020
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