The Cumulative Risk Assessment of Hepatotoxic Chemicals: A Hepatic Histopathology Perspective-Reference-Cited by-同舟云学术

The Cumulative Risk Assessment of Hepatotoxic Chemicals: A Hepatic Histopathology Perspective

Published:2020-01-14 Issue:3 Volume:48 Page:397-410
ISSN:0192-6233
Container-title:Toxicologic Pathology
language:en
Short-container-title:Toxicol Pathol

Author:

Foster John R.¹^ORCID,Semino-Beninel Giovanna²,Melching-Kollmuss Stephanie³

Affiliation:

1. Regulatory Science Associates, Kip Marina, Inverkip, Renfrewshire, United Kingdom

2. Bayer CropScience France, Crop Science, Regulatory Toxicology, Sophia Antipolis, France

3. BASF SE, Ludwigshafen am Rhein, Germany

Abstract

The increased concern on the consequence of exposure to multiple chemical combinations has led national regulatory authorities to develop different concepts to conduct risk assessments on chemical mixtures. Pesticide residues were identified as “problem formulation” in the respective European regulations and in this context, the European Food and Safety Authority has suggested to group pesticidal active ingredients (AIs) into cumulative assessment groups (CAGs) based on the toxicological properties of each AI. One proposed CAG, on the liver, currently consists of 15 subgroups, each representing a specific hepatotoxic effect observed in toxicity studies. Dietary cumulative risk assessments would then have to be conducted assuming dose additivity of all members of each CAG subgroup. The purpose of this publication is to group AIs based upon the knowledge of the pathogenesis of liver effects to discriminate between primary end points (direct consequence of chemical interaction with a biological target) and secondary end points (which are a consequence of, or that arise out of, a previous pathological change). Focusing on the relevant primary end points strengthens and simplifies the selection of compounds for cumulative risk assessment regarding the liver and better rationalizes the basis for chemical grouping. Relevant dose additivity is to be expected at the level of the primary/leading pathological end points and not at the level of the secondary end points. We recognize, however, that special consideration is needed for substances provoking neoplasia, and this category is included in the group of primary end points for which chemicals inducing them are grouped for risk assessment. Using the pathological basis for defining the respective CAGs, 6 liver subgroups and 2 gallbladder/bile duct groups are proposed. This approach simplifies the cumulative assessment calculation without obviously affecting consumer safety.

Funder

European Crop Protection Agency

Publisher

SAGE Publications

Subject

Cell Biology,Toxicology,Molecular Biology,Pathology and Forensic Medicine

Link

http://journals.sagepub.com/doi/pdf/10.1177/0192623319895481

Reference59 articles.

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