Your search keyword '"Widenfalk, Anneli"' showing total 10 results

1. Adherence to the EAT-Lancet diet in relation to mortality and exposure to food contaminants in population-based cohorts of Swedish men and women

Author

Pitt, Stephanie, Kałuża, Joanna, Widenfalk, Anneli, Åkesson, Agneta, and Wolk, Alicja

Published

2024

2. Associations between dietary pesticide residue mixture exposure and mortality in a population-based prospective cohort of men and women

Author

Åkesson, Agneta, Donat-Vargas, Carolina, Hallström, Elinor, Sonesson, Ulf, Widenfalk, Anneli, and Wolk, Alicja

Published

2023

3. Statement of the Scientific Panel on Plant Protection Products and their Residues (PPR Panel) on the design and conduct of groundwater monitoring studies supporting groundwater exposure assessments of pesticides

Author

EFSA PPR Panel (EFSA Panel on Plant Protection Products and their Residues), Hernández, Antonio García, Adriaanse, Paulien, Aldrich, Annette, Berny, Philippe, Coja, Tamara, Duquesne, Sabine, Focks, Andreas, Marinovich, Marina, Millet, Maurice, Pelkonen, Olavi, Pieper, Silvia, Topping, Christopher John, Widenfalk, Anneli, Wilks, Martin F, Wolterink, Gerrit, Kasteel, Roy, Kuppe, Konstantin, and Tiktak, Aaldrik

Published

2023

4. Scientific opinion on toxicity of pyrethroid common metabolites

Author

Hernandez-Jerez, Antonio F., Adriaanse, Paulien, Aldrich, Annette, Berny, Philippe, Duquesne, Sabine, Focks, Andreas, Marinovich, Marina, Millet, Maurice, Pelkonen, Olavi, Pieper, Silvia, Tiktak, Aaldrik, Topping, Christopher J., Widenfalk, Anneli, Wilks, Martin, Wolterink, Gerrit, Binaglia, Marco, Chiusolo, Arianna, Serafimova, Rositsa, Terron, Andrea, and Coja, Tamara

Subjects

3-phenoxybenzaldehyde, (geno)toxicity, health-based guidance values, 3-(4′-hydroxyphenoxy)benzoic acid, pyrethroid common metabolites, 3-phenoxybenzoic acid, pesticides residues

Abstract

The EFSA Panel on Plant Protection Products and their Residues was requested by the European Commission, to conclude based upon available evidence if metabolites 3-phenoxybenzoic acid (PBA) and 3-(4′-hydroxyphenoxy)benzoic acid (PBA(OH)), common to several pyrethroid compounds, have genotoxic properties, if they share the (neuro)toxicity profile of their parent compounds, and if evidence allows to conclude on their health-based guidance values. Available body of evidence consisted of studies from regulatory dossiers submissions, as well as from public literature. In addition, the data gap for short-term toxicity profile of PBA was addressed by read-across. Assessment revealed that PBA and PBA(OH) do not raise a concern with respect to genotoxicity. As regards general toxicity, PBA and PBA(OH) have different qualitative (no neurotoxic mechanism) and quantitative (higher NOAELs) toxicity compared to the parent pyrethroid compounds. For both metabolites, acceptable daily intake (ADI) and acute reference dose (ARfD) values were derived at 0.1 mg/kg body weight (bw) per day and 1 mg/kg bw, respectively.

Published

2022

5. Statement of the Scientific Panel on Plant Protection Products and their Residues (PPR Panel) on the design and conduct of groundwater monitoring studies supporting groundwater exposure assessments of pesticides.

Author

Hernandez‐Jerez, Antonio, Adriaanse, Paulien, Aldrich, Annette, Berny, Philippe, Coja, Tamara, Duquesne, Sabine, Focks, Andreas, Marinovich, Marina, Millet, Maurice, Pelkonen, Olavi, Pieper, Silvia, Topping, Christopher, Widenfalk, Anneli, Wilks, Martin, Wolterink, Gerrit, Kasteel, Roy, Kuppe, Konstantin, and Tiktak, Aaldrik

Subjects

GROUNDWATER monitoring, PLANT products, PLANT protection, GROUNDWATER, PESTICIDES

Abstract

Groundwater monitoring is the highest tier in the leaching assessment of plant protection products in the EU. The European Commission requested EFSA for a review by the PPR Panel of the scientific paper of Gimsing et al. (2019) on the design and conduct of groundwater monitoring studies. The Panel concludes that this paper provides many recommendations; however, specific guidance on how to design, conduct and evaluate groundwater monitoring studies for regulatory purposes is missing. The Panel notes that there is no agreed specific protection goal (SPG) at EU level. Also, the SPG has not yet been operationalised in an agreed exposure assessment goal (ExAG). The ExAG describes which groundwater needs to be protected, where and when. Because the design and interpretation of monitoring studies depends on the ExAG, development of harmonised guidance is not yet possible. The development of an agreed ExAG must therefore be given priority. A central question in the design and interpretation of groundwater monitoring studies is that of groundwater vulnerability. Applicants must demonstrate that the selected monitoring sites represent realistic worst‐case conditions as specified in the ExAG. Guidance and models are needed to support this step. A prerequisite for the regulatory use of monitoring data is the availability of complete data on the use history of the products containing the respective active substances. Applicants must further demonstrate that monitoring wells are hydrologically connected to the fields where the active substance has been applied. Modelling in combination with (pseudo)tracer experiments would be the preferred option. The Panel concludes that well‐conducted monitoring studies provide more realistic exposure assessments and can therefore overrule results from lower tier studies. Groundwater monitoring studies involve a high workload for both regulators and applicants. Standardised procedures and monitoring networks could help to reduce this workload. [ABSTRACT FROM AUTHOR]

Published

2023

6. Development of adverse outcome pathways relevant for the identification of substances having endocrine disruption properties Uterine adenocarcinoma as adverse outcome.

Author

Hernandez‐Jerez, Antonio F, Adriaanse, Paulien, Aldrich, Annette, Berny, Philippe, Coja, Tamara, Duquesne, Sabine, Focks, Andreas, Millet, Maurice, Pelkonen, Olavi, Pieper, Silvia, Tiktak, Aaldrik, Topping, Christopher J, Widenfalk, Anneli, Wilks, Martin, Wolterink, Gerrit, Angeli, Karine, Recordati, Camilla, Van Duursen, Majorie, Aiassa, Elisa, and Lanzoni, Anna

Subjects

ADENOCARCINOMA, ENDOCRINE disruptors, ESTROGEN receptors, LITERATURE reviews, ENDOMETRIUM, ORGANIC foods

Abstract

Development of adverse outcome pathways (AOPs) for uterine adenocarcinoma can provide a practical tool to implement the EFSA‐ECHA Guidance (2018) for the identification of endocrine disruptors in the context of Regulations (EU) No 528/2012 and (EC) No 1107/2009. AOPs can give indications about the strength of the relationship between an adverse outcome (intended as a human health outcome) and chemicals (pesticides but not only) affecting the pathways. In this scientific opinion, the PPR Panel explored the development of AOPs for uterine adenocarcinoma. An evidence‐based approach methodology was applied, and literature reviews were produced using a structured framework assuring transparency, objectivity, and comprehensiveness. Several AOPs were developed; these converged to a common critical node, that is increased estradiol availability in the uterus followed by estrogen receptor activation in the endometrium; therefore, a putative AOP network was considered. An uncertainty analysis and a probabilistic quantification of the weight of evidence have been carried out via expert knowledge elicitation for each set of MIEs/KEs/KERs included in individual AOPs. The collected data on the AOP network were evaluated qualitatively, whereas a quantitative uncertainty analysis for weight of the AOP network certainty has not been performed. Recommendations are provided, including exploring further the uncertainties identified in the AOPs and putative AOP network; further methodological developments for quantifying the certainty of the KERs and of the overall AOPs and AOP network; and investigating of NAMs applications in the context of some of the MIEs/KEs currently part of the putative AOP network developed. This publication is linked to the following EFSA Supporting Publications article: http://onlinelibrary.wiley.com/doi/10.2903/sp.efsa.2023.EN-7748/full [ABSTRACT FROM AUTHOR]

Published

2023

7. Associations between Dietary Pesticide Residue Mixture Exposure and Mortality in a Population-Based Prospective Cohort of Men and Women

Author

Akesson, Agneta, primary, Donat-Vargas, Carolina, additional, Hallström, Elinor, additional, Sonesson, Ulf, additional, Widenfalk, Anneli, additional, and Wolk, Alicja, additional

Published

2022

8. Scientific opinion on toxicity of pyrethroid common metabolites.

Author

Hernandez‐Jerez, Antonio F, Adriaanse, Paulien, Aldrich, Annette, Berny, Philippe, Duquesne, Sabine, Focks, Andreas, Marinovich, Marina, Millet, Maurice, Pelkonen, Olavi, Pieper, Silvia, Tiktak, Aaldrik, Topping, Christopher J, Widenfalk, Anneli, Wilks, Martin, Wolterink, Gerrit, Binaglia, Marco, Chiusolo, Arianna, Serafimova, Rositsa, Terron, Andrea, and Coja, Tamara

Subjects

PYRETHROIDS, METABOLITES, BENZOIC acid, PLANT products, PESTICIDE residues in food

Abstract

The EFSA Panel on Plant Protection Products and their Residues was requested by the European Commission, to conclude based upon available evidence if metabolites 3‐phenoxybenzoic acid (PBA) and 3‐(4′‐hydroxyphenoxy)benzoic acid (PBA(OH)), common to several pyrethroid compounds, have genotoxic properties, if they share the (neuro)toxicity profile of their parent compounds, and if evidence allows to conclude on their health‐based guidance values. Available body of evidence consisted of studies from regulatory dossiers submissions, as well as from public literature. In addition, the data gap for short‐term toxicity profile of PBA was addressed by read‐across. Assessment revealed that PBA and PBA(OH) do not raise a concern with respect to genotoxicity. As regards general toxicity, PBA and PBA(OH) have different qualitative (no neurotoxic mechanism) and quantitative (higher NOAELs) toxicity compared to the parent pyrethroid compounds. For both metabolites, acceptable daily intake (ADI) and acute reference dose (ARfD) values were derived at 0.1 mg/kg body weight (bw) per day and 1 mg/kg bw, respectively. [ABSTRACT FROM AUTHOR]

Published

2022

9. Statement on the active substance acetamiprid.

Author

Hernandez Jerez, Antonio, Adriaanse, Paulien, Berny, Philippe, Coja, Tamara, Duquesne, Sabine, Focks, Andreas, Marinovich, Marina, Millet, Maurice, Pelkonen, Olavi, Pieper, Silvia, Tiktak, Aaldrik, Topping, Christopher, Widenfalk, Anneli, Wilks, Martin, Wolterink, Gerrit, Rundlöf, Maj, Ippolito, Alessio, Linguadoca, Alberto, Martino, Laura, and Panzarea, Martina

Subjects

ANIMAL products, HUMAN ecology, SOIL biology, BEE products, ENDOCRINE disruptors, IDENTIFICATION documents, AQUATIC organisms

Abstract

Acetamiprid is a pesticide active substance with insecticidal action currently under the third renewal (AIR3) of the Commission implementing regulation (EU) No 844/2012. Following concerns that this substance may pose high risks to humans and the environment, the French authorities asked the Commission to restrict its uses under Article 69 of Regulation (EC) No 1107/2009. To support this request, competent Authorities from France cited a series of literature papers investigating its hazards and/or exposure to humans and the environment. Consequently, the EFSA PPR Panel was mandated to advise on the likelihood that body of evidence would constitute proof of serious risks to humans or the environment. Therefore, the EFSA PPR Panel evaluated the likelihood of these studies indicating new or higher hazards and exposure to humans and the environment compared to previous EU assessments.A stepwise methodology was designed, including: (i) the initial screening; (ii) the data extraction and critical appraisal based on the principles of OHAT/NTP; (iii) the weight of evidence, including consideration of the previous EU assessments; (iv) the uncertainty analysis, followed, whenever relevant, by an expert knowledge elicitation process. For human health, no conclusive evidence of higher hazards compared to previous assessment was found for genotoxicity, developmental toxicity, neurotoxicity including developmental neurotoxicity and immunotoxicity. However, due to the lack of adequate assessment of the current data set, the PPR Panel recommends conducting an assessment of endocrine disrupting properties for acetamiprid in line with EFSA/ECHA guidance document for the identification of endocrine disruptors. For environment, no conclusive, robust evidence of higher hazards compared to the previous assessment was found for birds, aquatic organisms, bees and soil organisms. However, the potential of high inter‐species sensitivity of birds and bees towards acetamiprid requires further consideration. This publication is linked to the following EFSA Journal article: http://onlinelibrary.wiley.com/doi/10.2903/j.efsa.2022.7030/full [ABSTRACT FROM AUTHOR]

Published

2022

10. Statement on the active substance flupyradifurone.

Author

Hernandez Jerez, Antonio, Adriaanse, Paulien, Berny, Philippe, Coja, Tamara, Duquesne, Sabine, Focks, Andreas, Marinovich, Marina, Millet, Maurice, Pelkonen, Olavi, Pieper, Silvia, Tiktak, Aaldrik, Topping, Christopher, Widenfalk, Anneli, Wilks, Martin, Wolterink, Gerrit, Rundlöf, Maj, Ippolito, Alessio, Linguadoca, Alberto, Martino, Laura, and Panzarea, Martina

Subjects

HONEYBEES, HUMAN ecology, PLANT products, PLANT protection, COMPETENT authority

Abstract

Flupyradifurone is a novel butenolide insecticide, first approved as an active substance for use in plant protection products by Commission Implementing Regulation (EU) 2015/2084. Following concerns that this substance may pose high risks to humans and the environment, the French authorities, in November 2020, asked the Commission to restrict its uses under Article 69 of Regulation (EC) No 1107/2009. To support this request, competent Authorities from France cited a series of literature papers investigating its hazards and/or exposure to humans and the environment. In addition, in June 2020, the Dutch Authorities notified the Commission, under Article 56 of Regulation (EC) No 1107/2009, of new information on flupyradifurone on the wild bee species Megachile rotundata. This notification is also referred to in the French notification on flupyradifurone. Consequently, the EFSA PPR Panel was mandated to quantify the likelihood of this body of evidence constituting proof of serious risks to humans or the environment. Therefore, the EFSA PPR Panel evaluated the likelihood of these studies indicating new or higher hazards and exposure to humans and the environment compared to previous EU assessments. A stepwise methodology was designed, including: (i) the initial screening; (ii) data extraction and critical appraisal based on the principles of OHAT/NTP; (iii) weight of evidence, including consideration of the previous EU assessments; (iv) uncertainty analysis, followed, whenever relevant, by an expert knowledge elicitation process. For the human health, only one study was considered relevant for the genotoxic potential of flupyradifurone in vitro. These data did not provide sufficient information to overrule the EU assessment, as in vivo studies already addressed the genotoxic potential of flupyradifurone. Environment: All available data investigated hazards in bee species. For honey bees, the likelihood of the new data indicating higher hazards than the previous EU assessment was considered low or moderate, with some uncertainties. However, among solitary bee species – which were not addressed in the previous EU assessment – there was evidence that Megachile rotundata may be disproportionately sensitive to flupyradifurone. This sensitivity, which may partially be explained by the low bodyweight of this species, was mechanistically linked to inadequate bodily metabolisation processes. This publication is linked to the following EFSA Journal article: http://onlinelibrary.wiley.com/doi/10.2903/j.efsa.2022.7031/full [ABSTRACT FROM AUTHOR]

Published

2022