Differential Radiosensitivity Phenotypes of DNA-PKcs Mutations Affecting NHEJ and HRR Systems following Irradiation with Gamma-Rays or Very Low Fluences of Alpha Particles | Zendy

YuFen Lin | Zendy; Hatsumi Nagasawa | Zendy; John B. Little | Zendy; Takamitsu A. Kato | Zendy; Hung-Ying Shih | Zendy; Xian-Jin Xie | Zendy; Paul F. Wilson | Zendy; John Brogan | Zendy; Akihiro Kurimasa | Zendy; David J. Chen | Zendy; Joel S. Bedford | Zendy; Benjamin P.C. Chen | Zendy

Open Access

Differential Radiosensitivity Phenotypes of DNA-PKcs Mutations Affecting NHEJ and HRR Systems following Irradiation with Gamma-Rays or Very Low Fluences of Alpha Particles

Author(s) -

YuFen Lin,

Hatsumi Nagasawa,

John B. Little,

Takamitsu A. Kato,

Hung-Ying Shih,

Xian-Jin Xie,

Paul F. Wilson,

John Brogan,

Akihiro Kurimasa,

David J. Chen,

Joel S. Bedford,

Benjamin P.C. Chen

Publication year - 2014

Publication title -

plos one

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.99

H-Index - 332

ISSN - 1932-6203

DOI - 10.1371/journal.pone.0093579

Subject(s) - dna pkcs , microbiology and biotechnology , mutant , biology , ku80 , dna repair , dna damage , radiosensitivity , homologous recombination , cell cycle , wild type , null cell , dna , cell culture , cell , genetics , gene , irradiation , dna binding protein , physics , transcription factor , nuclear physics

We have examined cell-cycle dependence of chromosomal aberration induction and cell killing after high or low dose-rate γ irradiation in cells bearing DNA-PKcs mutations in the S2056 cluster, the T2609 cluster, or the kinase domain. We also compared sister chromatid exchanges (SCE) production by very low fluences of α-particles in DNA-PKcs mutant cells, and in homologous recombination repair (HRR) mutant cells including Rad51C, Rad51D, and Fancg/xrcc9. Generally, chromosomal aberrations and cell killing by γ-rays were similarly affected by mutations in DNA-PKcs, and these mutant cells were more sensitive in G 1 than in S/G 2 phase. In G 1 -irradiated DNA-PKcs mutant cells, both chromosome- and chromatid-type breaks and exchanges were in excess than wild-type cells. For cells irradiated in late S/G 2 phase, mutant cells showed very high yields of chromatid breaks compared to wild-type cells. Few exchanges were seen in DNA-PKcs-null, Ku80-null, or DNA-PKcs kinase dead mutants, but exchanges in excess were detected in the S2506 or T2609 cluster mutants. SCE induction by very low doses of α-particles is resulted from bystander effects in cells not traversed by α-particles. SCE seen in wild-type cells was completely abolished in Rad51C- or Rad51D-deficient cells, but near normal in Fancg/xrcc9 cells. In marked contrast, very high levels of SCEs were observed in DNA-PKcs-null, DNA-PKcs kinase-dead and Ku80-null mutants. SCE induction was also abolished in T2609 cluster mutant cells, but was only slightly reduced in the S2056 cluster mutant cells. Since both non-homologous end-joining (NHEJ) and HRR systems utilize initial DNA lesions as a substrate, these results suggest the possibility of a competitive interference phenomenon operating between NHEJ and at least the Rad51C/D components of HRR; the level of interaction between damaged DNA and a particular DNA-PK component may determine the level of interaction of such DNA with a relevant HRR component.

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