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Nejvíce citované: 27554597

2 citací v PubMed Filtry

Nejvíce citovaný článek - PubMed ID 27554597

Záznam nenalezen v Medvik. Navštivte PubMed 27554597

Článek

New approach methodologies to facilitate and improve the hazard assessment of non-genotoxic carcinogens-a PARC project

Audebert, Marc
Autor Audebert, Marc INRAE: Toxalim, INRAE, INP-ENVT, INP-EI-Purpan, Université de Toulouse 3 Paul Sabatier, Toulouse, France
Assmann, Ann-Sophie
Autor Assmann, Ann-Sophie Department Experimental Toxicology and ZEBET, German Centre for the Protection of Laboratory Animals (Bf3R) and Department Food Safety, BfR: German Federal Institute for Risk Assessment, Berlin, Germany
Azqueta, Amaya
Autor Azqueta, Amaya Department of Pharmacology and Toxicology, School of Pharmacy and Nutrition, UNAV: University of Navarra, Pamplona, Spain
Babica, Pavel
Autor Babica, Pavel RECETOX: RECETOX, Faculty of Science, Masaryk University, Brno, Czechia
Benfenati, Emilio
Autor Benfenati, Emilio IRFMN: Istituto di Ricerche Farmacologiche Mario Negri-IRCCS, Milan, Italy
Bortoli, Sylvie
Autor Bortoli, Sylvie INSERM: INSERM UMR-S 1124 T3S-Université Paris Cité, Paris, France
Bouwman, Peter
Autor Bouwman, Peter UL-LACDR: Leiden Academic Centre for Drug Research, Leiden University, Leiden, Netherlands
Braeuning, Albert
Autor Braeuning, Albert Department Experimental Toxicology and ZEBET, German Centre for the Protection of Laboratory Animals (Bf3R) and Department Food Safety, BfR: German Federal Institute for Risk Assessment, Berlin, Germany
Burgdorf, Tanja
Autor Burgdorf, Tanja Department Experimental Toxicology and ZEBET, German Centre for the Protection of Laboratory Animals (Bf3R) and Department Food Safety, BfR: German Federal Institute for Risk Assessment, Berlin, Germany
Coumoul, Xavier
Autor Coumoul, Xavier INSERM: INSERM UMR-S 1124 T3S-Université Paris Cité, Paris, France

Frontiers in toxicology. 2023 ; 5 () : 1220998. [epub] 20230710

Front Toxicol
ISSN 2673-3080
Zdroj

Carcinogenic chemicals, or their metabolites, can be classified as genotoxic or non-genotoxic carcinogens (NGTxCs). Genotoxic compounds induce DNA damage, which can be detected by an established in vitro and in vivo battery of genotoxicity assays. For NGTxCs, DNA is not the primary target, and the possible modes of action (MoA) of NGTxCs are much more diverse than those of genotoxic compounds, and there is no specific in vitro assay for detecting NGTxCs. Therefore, the evaluation of the carcinogenic potential is still dependent on long-term studies in rodents. This 2-year bioassay, mainly applied for testing agrochemicals and pharmaceuticals, is time-consuming, costly and requires very high numbers of animals. More importantly, its relevance for human risk assessment is questionable due to the limited predictivity for human cancer risk, especially with regard to NGTxCs. Thus, there is an urgent need for a transition to new approach methodologies (NAMs), integrating human-relevant in vitro assays and in silico tools that better exploit the current knowledge of the multiple processes involved in carcinogenesis into a modern safety assessment toolbox. Here, we describe an integrative project that aims to use a variety of novel approaches to detect the carcinogenic potential of NGTxCs based on different mechanisms and pathways involved in carcinogenesis. The aim of this project is to contribute suitable assays for the safety assessment toolbox for an efficient and improved, internationally recognized hazard assessment of NGTxCs, and ultimately to contribute to reliable mechanism-based next-generation risk assessment for chemical carcinogens.

Klíčová slova
NAM, NGTxC, PARC, new approach methodologies, non-genotoxic carcinogens,
Publikační typ
časopisecké články MeSH
přehledy MeSH

Článek

Adaptation of the in vitro micronucleus assay for genotoxicity testing using 3D liver models supporting longer-term exposure durations

Mutagenesis. 2020 Sep 12 ; 35 (4) : 319-330.

ISSN 1464-3804 | 0267-8357
Zdroj

Following advancements in the field of genotoxicology, it has become widely accepted that 3D models are not only more physiologically relevant but also have the capacity to elucidate more complex biological processes that standard 2D monocultures are unable to. Whilst 3D liver models have been developed to evaluate the short-term genotoxicity of chemicals, the aim of this study was to develop a 3D model that could be used with the regulatory accepted in vitro micronucleus (MN) following low-dose, longer-term (5 days) exposure to engineered nanomaterials (ENMs). A comparison study was carried out between advanced models generated from two commonly used liver cell lines, namely HepaRG and HepG2, in spheroid format. While both spheroid systems displayed good liver functionality and viability over 14 days, the HepaRG spheroids lacked the capacity to actively proliferate and, therefore, were considered unsuitable for use with the MN assay. This study further demonstrated the efficacy of the in vitro 3D HepG2 model to be used for short-term (24 h) exposures to genotoxic chemicals, aflatoxin B1 (AFB1) and methyl-methanesulfonate (MMS). The 3D HepG2 liver spheroids were shown to be more sensitive to DNA damage induced by AFB1 and MMS when compared to the HepG2 2D monoculture. This 3D model was further developed to allow for longer-term (5 day) ENM exposure. Four days after seeding, HepG2 spheroids were exposed to Zinc Oxide ENM (0-2 µg/ml) for 5 days and assessed using both the cytokinesis-block MN (CBMN) version of the MN assay and the mononuclear MN assay. Following a 5-day exposure, differences in MN frequency were observed between the CBMN and mononuclear MN assay, demonstrating that DNA damage induced within the first few cell cycles is distributed across the mononucleated cell population. Together, this study demonstrates the necessity to adapt the MN assay accordingly, to allow for the accurate assessment of genotoxicity following longer-term, low-dose ENM exposure.

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