Reduced Activity of Double-Strand Break Repair Genes in Prostate Cancer Patients With Late Normal Tissue Radiation Toxicity

Article ID	Journal	Published Year	Pages	File Type
8220214	International Journal of Radiation OncologyBiologyPhysics	2014	7 Pages	PDF

Abstract

Both gene expression profiling and DNA DSB repair kinetics data imply that less-efficient repair of radiation-induced DSBs may contribute to the development of late normal tissue damage. Induction levels of DSB repair genes (eg, RAD51) may potentially be used to assess the risk for late radiation toxicity.

Related Topics

Physical Sciences and Engineering Physics and Astronomy Radiation

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Reduced Activity of Double-Strand Break Repair Genes in Prostate Cancer Patients With Late Normal Tissue Radiation Toxicity

Authors

Bregje MSc, Suzanne E. MSc, Perry D. PhD, Jan Paul PhD, Lukas J.A. MD, PhD, Harry PhD, Nicolaas A.P. PhD,