DNA Double-Strand Breaks Induced in Human Cells by Twelve Metallic Species: Quantitative Inter-Comparisons and Influence of the ATM Protein

Despite a considerable amount of data, the molecular and cellular bases of the toxicity due to metal exposure remain unknown. Recent mechanistic models from radiobiology have emerged, pointing out that the radiation-induced nucleo-shuttling of the ATM protein (RIANS) initiates the recognition and th...

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Autores principales: Viau, Muriel, Sonzogni, Laurène, Ferlazzo, Mélanie L., Berthel, Elise, Pereira, Sandrine, Bodgi, Larry, Granzotto, Adeline, Devic, Clément, Fervers, Béatrice, Charlet, Laurent, Foray, Nicolas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8533583/
https://www.ncbi.nlm.nih.gov/pubmed/34680095
http://dx.doi.org/10.3390/biom11101462
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author Viau, Muriel
Sonzogni, Laurène
Ferlazzo, Mélanie L.
Berthel, Elise
Pereira, Sandrine
Bodgi, Larry
Granzotto, Adeline
Devic, Clément
Fervers, Béatrice
Charlet, Laurent
Foray, Nicolas
author_facet Viau, Muriel
Sonzogni, Laurène
Ferlazzo, Mélanie L.
Berthel, Elise
Pereira, Sandrine
Bodgi, Larry
Granzotto, Adeline
Devic, Clément
Fervers, Béatrice
Charlet, Laurent
Foray, Nicolas
author_sort Viau, Muriel
collection PubMed
description Despite a considerable amount of data, the molecular and cellular bases of the toxicity due to metal exposure remain unknown. Recent mechanistic models from radiobiology have emerged, pointing out that the radiation-induced nucleo-shuttling of the ATM protein (RIANS) initiates the recognition and the repair of DNA double-strand breaks (DSB) and the final response to genotoxic stress. In order to document the role of ATM-dependent DSB repair and signalling after metal exposure, we applied twelve different metal species representing nine elements (Al, Cu, Zn Ni, Pd, Cd, Pb, Cr, and Fe) to human skin, mammary, and brain cells. Our findings suggest that metals may directly or indirectly induce DSB at a rate that depends on the metal properties and concentration, and tissue type. At specific metal concentration ranges, the nucleo-shuttling of ATM can be delayed which impairs DSB recognition and repair and contributes to toxicity and carcinogenicity. Interestingly, as observed after low doses of ionizing radiation, some phenomena equivalent to the biological response observed at high metal concentrations may occur at lower concentrations. A general mechanistic model of the biological response to metal exposure based on the nucleo-shuttling of ATM is proposed to describe the metal-induced stress response and to define quantitative endpoints for toxicity and carcinogenicity.
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spelling pubmed-85335832021-10-23 DNA Double-Strand Breaks Induced in Human Cells by Twelve Metallic Species: Quantitative Inter-Comparisons and Influence of the ATM Protein Viau, Muriel Sonzogni, Laurène Ferlazzo, Mélanie L. Berthel, Elise Pereira, Sandrine Bodgi, Larry Granzotto, Adeline Devic, Clément Fervers, Béatrice Charlet, Laurent Foray, Nicolas Biomolecules Article Despite a considerable amount of data, the molecular and cellular bases of the toxicity due to metal exposure remain unknown. Recent mechanistic models from radiobiology have emerged, pointing out that the radiation-induced nucleo-shuttling of the ATM protein (RIANS) initiates the recognition and the repair of DNA double-strand breaks (DSB) and the final response to genotoxic stress. In order to document the role of ATM-dependent DSB repair and signalling after metal exposure, we applied twelve different metal species representing nine elements (Al, Cu, Zn Ni, Pd, Cd, Pb, Cr, and Fe) to human skin, mammary, and brain cells. Our findings suggest that metals may directly or indirectly induce DSB at a rate that depends on the metal properties and concentration, and tissue type. At specific metal concentration ranges, the nucleo-shuttling of ATM can be delayed which impairs DSB recognition and repair and contributes to toxicity and carcinogenicity. Interestingly, as observed after low doses of ionizing radiation, some phenomena equivalent to the biological response observed at high metal concentrations may occur at lower concentrations. A general mechanistic model of the biological response to metal exposure based on the nucleo-shuttling of ATM is proposed to describe the metal-induced stress response and to define quantitative endpoints for toxicity and carcinogenicity. MDPI 2021-10-05 /pmc/articles/PMC8533583/ /pubmed/34680095 http://dx.doi.org/10.3390/biom11101462 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Viau, Muriel
Sonzogni, Laurène
Ferlazzo, Mélanie L.
Berthel, Elise
Pereira, Sandrine
Bodgi, Larry
Granzotto, Adeline
Devic, Clément
Fervers, Béatrice
Charlet, Laurent
Foray, Nicolas
DNA Double-Strand Breaks Induced in Human Cells by Twelve Metallic Species: Quantitative Inter-Comparisons and Influence of the ATM Protein
title DNA Double-Strand Breaks Induced in Human Cells by Twelve Metallic Species: Quantitative Inter-Comparisons and Influence of the ATM Protein
title_full DNA Double-Strand Breaks Induced in Human Cells by Twelve Metallic Species: Quantitative Inter-Comparisons and Influence of the ATM Protein
title_fullStr DNA Double-Strand Breaks Induced in Human Cells by Twelve Metallic Species: Quantitative Inter-Comparisons and Influence of the ATM Protein
title_full_unstemmed DNA Double-Strand Breaks Induced in Human Cells by Twelve Metallic Species: Quantitative Inter-Comparisons and Influence of the ATM Protein
title_short DNA Double-Strand Breaks Induced in Human Cells by Twelve Metallic Species: Quantitative Inter-Comparisons and Influence of the ATM Protein
title_sort dna double-strand breaks induced in human cells by twelve metallic species: quantitative inter-comparisons and influence of the atm protein
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8533583/
https://www.ncbi.nlm.nih.gov/pubmed/34680095
http://dx.doi.org/10.3390/biom11101462
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