DNA damage interactions on both nanometer and micrometer scale determine overall cellular damage

Author:

Friedrich Thomas,Ilicic Katarina,Greubel Christoph,Girst Stefanie,Reindl Judith,Sammer Matthias,Schwarz Benjamin,Siebenwirth Christian,Walsh Dietrich W. M.,Schmid Thomas E.,Scholz Michael,Dollinger Günther

Abstract

Abstract DNA double strand breaks (DSB) play a pivotal role for cellular damage, which is a hazard encountered in toxicology and radiation protection, but also exploited e.g. in eradicating tumors in radiation therapy. It is still debated whether and in how far clustering of such DNA lesions leads to an enhanced severity of induced damage. Here we investigate - using focused spots of ionizing radiation as damaging agent - the spatial extension of DNA lesion patterns causing cell inactivation. We find that clustering of DNA damage on both the nm and µm scale leads to enhanced inactivation compared to more homogeneous lesion distributions. A biophysical model interprets these observations in terms of enhanced DSB production and DSB interaction, respectively. We decompose the overall effects quantitatively into contributions from these lesion formation processes, concluding that both processes coexist and need to be considered for determining the resulting damage on the cellular level.

Funder

Bundesministerium für Bildung und Forschung

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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