The toxicity of tritium is a public health concern given its presence and mobility in the environment. For risk predictions using radiological protection models, it is essential to allocate an appropriate radiation weighting factor (WR). This in turn should be consistent with the observed relative biological effectiveness (RBE) of tritium beta radiation. Although the International Commission on Radiological Protection (ICRP) currently recommends a WR of 1 for the calculation of committed effective dose for X rays, gamma rays and electrons of all energies, including tritium energies, there are concerns that tritium health risks are underestimated and that current regulatory tritium drinking water standards need revision. In this study, we investigated potential cytotoxic and genotoxic effects in mouse spleen after one month and eight months of chronic exposure to low-dose tritiated water (HTO). The dose regimes studied were designed to mimic human chronic consumption of HTO at levels of 10 kBq/l, 1 MBq/l and 20 MBq/l. The total doses from these radiation exposures ranged from 0.01 to 180 mGy. We also compared the biological effects of exposure to HTO with equivalent exposure to external whole-body 60Co gamma rays. Changes in spleen weight and somatic intrachromosomal recombination (DNA inversions) in spleen tissue of pKZ1Tg/+ mice were monitored. Our results showed no overall changes in either spleen organ weights and no increase mouse splenic intrachromosomal recombination frequencies, indicating that current drinking water standards for tritium exposure in the form of HTO are likely to be adequately protective against cytotoxic and genotoxic damage in spleen. These results demonstrate no evidence for cytotoxicity or genotoxicity in mouse spleen following chronic exposures to HTO activities (or equivalent gamma doses) up to 20 MBq/L.
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1 December 2016
REGULAR ARTICLES|
December 06 2016
Environmentally Relevant Chronic Low-Dose Tritium and Gamma Exposures do not Increase Somatic Intrachromosomal Recombination in pKZ1 Mouse Spleen
Laura Bannister;
Laura Bannister
1
aCanadian Nuclear Laboratories, Chalk River, Ontario, Canada
1Address for correspondence: Canadian Nuclear Laboratories, Chalk River, ON, Canada; email: laura.bannister@cnl.ca.
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Mandy Serran;
Mandy Serran
aCanadian Nuclear Laboratories, Chalk River, Ontario, Canada
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Lindsey Bertrand;
Lindsey Bertrand
aCanadian Nuclear Laboratories, Chalk River, Ontario, Canada
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Dmitry Klokov;
Dmitry Klokov
aCanadian Nuclear Laboratories, Chalk River, Ontario, Canada
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Heather Wyatt;
Heather Wyatt
aCanadian Nuclear Laboratories, Chalk River, Ontario, Canada
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Melinda Blimkie;
Melinda Blimkie
aCanadian Nuclear Laboratories, Chalk River, Ontario, Canada
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Yann Gueguen;
Yann Gueguen
bInstitut de Radioprotection et de Sûreté Nucléaire (IRSN), PRP-HOM, Fontenay-aux-Roses, France
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Nicholas Priest;
Nicholas Priest
aCanadian Nuclear Laboratories, Chalk River, Ontario, Canada
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Jean-René Jourdain;
Jean-René Jourdain
bInstitut de Radioprotection et de Sûreté Nucléaire (IRSN), PRP-HOM, Fontenay-aux-Roses, France
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Pamela Sykes
Pamela Sykes
cFlinders Centre for Innovation in Cancer, Flinders University of South Australia, SA, Australia
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Radiat Res (2016) 186 (6): 539–548.
Citation
Laura Bannister, Mandy Serran, Lindsey Bertrand, Dmitry Klokov, Heather Wyatt, Melinda Blimkie, Yann Gueguen, Nicholas Priest, Jean-René Jourdain, Pamela Sykes; Environmentally Relevant Chronic Low-Dose Tritium and Gamma Exposures do not Increase Somatic Intrachromosomal Recombination in pKZ1 Mouse Spleen. Radiat Res 1 December 2016; 186 (6): 539–548. doi: https://doi.org/10.1667/RR14564.1
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