Influence of nuclear structure on the formation of radiation-induced lethal lesions

Purpose The rejoining of fragmented nuclear DNA caused by ionizing radiation may lead to lethal chromosome rearrangements, such as rings or dicentrics. The clinically useful linear quadratic relationship between dose and cell survival has been interpreted as the generation of lethal lesions secondar...

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Veröffentlicht in:International journal of radiation biology Jg. 92; H. 5; S. 229 - 240
Hauptverfasser: Friedman, Daniel A., Tait, Lauren, Vaughan, Andrew T. M.
Format: Journal Article
Sprache:Englisch
Veröffentlicht: England Taylor & Francis 03.05.2016
Schlagworte:
Animals
Apoptosis - genetics
Apoptosis - radiation effects
Cell Nucleus - physiology
Cell Nucleus - radiation effects
Cellular radiobiology
chromosome abberations
Chromosome Aberrations - radiation effects
Computer Simulation
DNA - genetics
DNA - radiation effects
DNA Damage - physiology
Dose-Response Relationship, Radiation
double-strand breaks
Evidence-Based Medicine
Humans
microdosimetry
models of cell killing
Models, Genetic
molecular radiobiology
Radiation Dosage
Cellular radiobiology
microdosimetry
chromosome abberations
molecular radiobiology
double-strand breaks
models of cell killing
ISSN:0955-3002, 1362-3095, 1362-3095
Online-Zugang:Volltext
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Zusammenfassung:Purpose The rejoining of fragmented nuclear DNA caused by ionizing radiation may lead to lethal chromosome rearrangements, such as rings or dicentrics. The clinically useful linear quadratic relationship between dose and cell survival has been interpreted as the generation of lethal lesions secondary to damage occurring in two separate chromosomes simultaneously (α component), or as potentially repairable separate events (β component). Here, the generation of such lesions is discussed, synthesizing existing knowledge with new insights gleaned from spatial proximity data made possible by high-throughput sequencing of chromosome conformation capture experiments. Over a range of several Mbp, the linear DNA strand is organized as a fractal globule generating multiple sites of contact that may facilitate deletions or inversions if the points of contact are damaged. On a larger scale, transcriptionally active euchromatin occupies a physically identifiable space separate from inactive areas and is preferentially susceptible to free radical attack after irradiation. Specific transcriptional programs link genomic locations within that space, potentially enhancing their interaction if subject to simultaneous fragmentation by a single radiation event. Conclusions High throughput spatial analysis of the factors that control chromosome proximity has the potential to better describe the formation of the lethal chromosome aberrations that kill irradiated cells.
Bibliographie:ObjectType-Article-1
SourceType-Scholarly Journals-1
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ISSN:0955-3002
1362-3095
1362-3095
DOI:10.3109/09553002.2016.1144941