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Resistance of hypoxic cells to ionizing radiation is influenced by homologous recombination status.

Debbie Sprong ,
Hilde L Janssen ,
Conchita Vens ,
Adrian C Begg

Abstract

METHODS AND MATERIALS

Chinese hamster cell lines with mutations in homologous recombination (XRCC2, XRCC3, BRAC2, RAD51C) or nonhomologous end-joining (DNA-PKcs) genes were irradiated under normoxic (20% oxygen) and hypoxic (<0.1% oxygen) conditions, and the oxygen enhancement ratio (OER) was calculated. In addition, Fanconi anemia fibroblasts (complementation groups C and G) were compared with fibroblasts from nonsyndrome patients. RAD51 foci were studied using immunofluorescence.

CONCLUSION

Homologous recombination plays an important role in determining hypoxic cell radiosensitivity. Lower OERs have also been reported in cells deficient in XPF and ERCC1, which, similar to homologous recombination genes, are known to play a role in cross-link repair. Because Fanconi anemia cells are also sensitive to cross-linking agents, this strengthens the notion that the capacity to repair cross-links determines hypoxic radiosensitivity.

RESULTS

All hamster cell lines deficient in homologous recombination showed a decrease in OER (1.5-2.0 vs. 2.6-3.0 for wild-types). In contrast, the OER for the DNA-PKcs-deficient line was comparable to wild-type controls. The two Fanconi anemia cell strains also showed a significant reduction in OER. The OER for RAD51 foci formation at late times after irradiation was considerably lower than that for survival in wild-type cells.

PURPOSE

To determine the role of DNA repair in hypoxic radioresistance.

More about this publication

International journal of radiation oncology, biology, physics

Volume 64
Issue nr. 2
Pages 562-72
Publication date 01-02-2006

Full text links

Publisher website (DOI) 10.1016/j.ijrobp.2005.09.031
Europe PubMed Central 16343804
Pubmed 16343804

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