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Primary and secondary clustering of DSB repair foci and repair kinetics compared for γ-rays, protons of different energies and high-LET (20)Ne ions

Purpose: Ionizing radiations of different qualities (e.g. high-LET and low-LET) might differently interact with structurally and functionally distinct higher order chromatin domains (discussed in [ 1] and citations therein); this might be reflected by DNA double strand break (DSB) repair efficiency...

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Autores principales: Falk, Martin, Lukasova, Emilie, Falkova, Iva, Davidkova, Marie, Bacikova, Alena, Stefancikova, Lenka, Jezkova, Lucie, Vachelova, Jana, Michaelidesova, Anna, Boreyko, Alla, Krasavin, Evgeny A., Kozubek, Stanislav
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3941551/
http://dx.doi.org/10.1093/jrr/rrt210
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author Falk, Martin
Lukasova, Emilie
Falkova, Iva
Davidkova, Marie
Bacikova, Alena
Stefancikova, Lenka
Jezkova, Lucie
Vachelova, Jana
Michaelidesova, Anna
Boreyko, Alla
Krasavin, Evgeny A.
Kozubek, Stanislav
author_facet Falk, Martin
Lukasova, Emilie
Falkova, Iva
Davidkova, Marie
Bacikova, Alena
Stefancikova, Lenka
Jezkova, Lucie
Vachelova, Jana
Michaelidesova, Anna
Boreyko, Alla
Krasavin, Evgeny A.
Kozubek, Stanislav
author_sort Falk, Martin
collection PubMed
description Purpose: Ionizing radiations of different qualities (e.g. high-LET and low-LET) might differently interact with structurally and functionally distinct higher order chromatin domains (discussed in [ 1] and citations therein); this might be reflected by DNA double strand break (DSB) repair efficiency and the mechanism of how cancerogenous chromosomal translocations (CHT) form. Therefore, we compared the DSB repair kinetics and formation of γH2AX/p53BP1 repair clusters upon the action of γ-rays [ 2, 3], protons (15 and 30 MeV) [ 4], and (20)Ne ions (preliminary data). Consequently, we discuss biological impacts of these clusters. Material and methods: Immunostaining methods in combination with high-resolution confocal microscopy, performed on 3D-fixed normal human skin fibroblasts [ 2– 4], were used to study initial distributions of γH2AX and p53BP1 repair foci and their changes during the post-irradiation (PI) time, with a special concern on foci clustering. Irradiations with γ-rays, protons of different energies (15 and 30 MeV), and high-LET (20)Ne ions was performed in IBP ASCR Brno (CR), NPI AVCR Řež (CR) and JINR Dubna (Russia), respectively. Results: Upon irradiating cells with (20)Ne ions, tracks of multiple clustered γH2AX and p53BP1 repair foci appeared immediately after the irradiation; these clusters, called here as the ‘primary clusters’, were rare in cells irradiated with γ-rays or protons (submitted). Though γH2AX/p53BP1 foci were positionally quite stable [ 2], ‘secondary clusters’ occasionally appeared after all kinds of irradiation during about 30 min PI. The formation of secondary clusters usually appeared due to the heterochromatin decondensation at the sites of heterochromatic DNA double-strand breaks (hcDSBs), followed by their protrusion into a limited space of nuclear subdomains of low density-chromatin (discussed in [ 1, 2, 5]). Conclusions: Primary clusters appear in cell nuclei immediately PI as the consequence of highly localized energy deposition, while secondary clusters develop during (and because of) DSB repair. Primary DSB clusters probably represent the main cause of chromosomal translocations induced with high-LET radiations while secondary clusters seem to be more important for low-LET γ-rays and protons. Secondary clusters of primary clusters (higher-order clusters) observed for (20)Ne ions might explain frequent formation of complex translocations upon the action of high-LET radiations. Finally, we suggest [ 1, 2, 4] a model that describes the relationship between the higher order chromatin structure, DSB formation, repair and misrepair.
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spelling pubmed-39415512014-03-04 Primary and secondary clustering of DSB repair foci and repair kinetics compared for γ-rays, protons of different energies and high-LET (20)Ne ions Falk, Martin Lukasova, Emilie Falkova, Iva Davidkova, Marie Bacikova, Alena Stefancikova, Lenka Jezkova, Lucie Vachelova, Jana Michaelidesova, Anna Boreyko, Alla Krasavin, Evgeny A. Kozubek, Stanislav J Radiat Res Poster Session 01: DNA Damage and Repair Purpose: Ionizing radiations of different qualities (e.g. high-LET and low-LET) might differently interact with structurally and functionally distinct higher order chromatin domains (discussed in [ 1] and citations therein); this might be reflected by DNA double strand break (DSB) repair efficiency and the mechanism of how cancerogenous chromosomal translocations (CHT) form. Therefore, we compared the DSB repair kinetics and formation of γH2AX/p53BP1 repair clusters upon the action of γ-rays [ 2, 3], protons (15 and 30 MeV) [ 4], and (20)Ne ions (preliminary data). Consequently, we discuss biological impacts of these clusters. Material and methods: Immunostaining methods in combination with high-resolution confocal microscopy, performed on 3D-fixed normal human skin fibroblasts [ 2– 4], were used to study initial distributions of γH2AX and p53BP1 repair foci and their changes during the post-irradiation (PI) time, with a special concern on foci clustering. Irradiations with γ-rays, protons of different energies (15 and 30 MeV), and high-LET (20)Ne ions was performed in IBP ASCR Brno (CR), NPI AVCR Řež (CR) and JINR Dubna (Russia), respectively. Results: Upon irradiating cells with (20)Ne ions, tracks of multiple clustered γH2AX and p53BP1 repair foci appeared immediately after the irradiation; these clusters, called here as the ‘primary clusters’, were rare in cells irradiated with γ-rays or protons (submitted). Though γH2AX/p53BP1 foci were positionally quite stable [ 2], ‘secondary clusters’ occasionally appeared after all kinds of irradiation during about 30 min PI. The formation of secondary clusters usually appeared due to the heterochromatin decondensation at the sites of heterochromatic DNA double-strand breaks (hcDSBs), followed by their protrusion into a limited space of nuclear subdomains of low density-chromatin (discussed in [ 1, 2, 5]). Conclusions: Primary clusters appear in cell nuclei immediately PI as the consequence of highly localized energy deposition, while secondary clusters develop during (and because of) DSB repair. Primary DSB clusters probably represent the main cause of chromosomal translocations induced with high-LET radiations while secondary clusters seem to be more important for low-LET γ-rays and protons. Secondary clusters of primary clusters (higher-order clusters) observed for (20)Ne ions might explain frequent formation of complex translocations upon the action of high-LET radiations. Finally, we suggest [ 1, 2, 4] a model that describes the relationship between the higher order chromatin structure, DSB formation, repair and misrepair. Oxford University Press 2014-03 /pmc/articles/PMC3941551/ http://dx.doi.org/10.1093/jrr/rrt210 Text en © The Author 2014. Published by Oxford University Press on behalf of The Japan Radiation Research Society and Japanese Society for Therapeutic Radiology and Oncology. http://creativecommons.org/licenses/by/3.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/3.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Poster Session 01: DNA Damage and Repair
Falk, Martin
Lukasova, Emilie
Falkova, Iva
Davidkova, Marie
Bacikova, Alena
Stefancikova, Lenka
Jezkova, Lucie
Vachelova, Jana
Michaelidesova, Anna
Boreyko, Alla
Krasavin, Evgeny A.
Kozubek, Stanislav
Primary and secondary clustering of DSB repair foci and repair kinetics compared for γ-rays, protons of different energies and high-LET (20)Ne ions
title Primary and secondary clustering of DSB repair foci and repair kinetics compared for γ-rays, protons of different energies and high-LET (20)Ne ions
title_full Primary and secondary clustering of DSB repair foci and repair kinetics compared for γ-rays, protons of different energies and high-LET (20)Ne ions
title_fullStr Primary and secondary clustering of DSB repair foci and repair kinetics compared for γ-rays, protons of different energies and high-LET (20)Ne ions
title_full_unstemmed Primary and secondary clustering of DSB repair foci and repair kinetics compared for γ-rays, protons of different energies and high-LET (20)Ne ions
title_short Primary and secondary clustering of DSB repair foci and repair kinetics compared for γ-rays, protons of different energies and high-LET (20)Ne ions
title_sort primary and secondary clustering of dsb repair foci and repair kinetics compared for γ-rays, protons of different energies and high-let (20)ne ions
topic Poster Session 01: DNA Damage and Repair
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3941551/
http://dx.doi.org/10.1093/jrr/rrt210
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