Journal
ENVIRONMENTAL AND MOLECULAR MUTAGENESIS
Volume 46, Issue 4, Pages 207-220Publisher
WILEY-LISS
DOI: 10.1002/em.20143
Keywords
T lymphocyte; human mutation; HPRT mutation; ionizing radiation; translocation
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Funding
- NCI NIH HHS [P30CA22435] Funding Source: Medline
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In an effort to mimic human in vivo exposures to ionizing irradiation, Go phase T lymphocytes from human peripheral blood samples were utilized for in vitro studies of the genotoxic effects of Cs-137 low-LET irradiation and Rn-222 high-LET irradiation. Both types of radiation induced mutations in the HPRT gene in a dose-dependent manner, with a mutant frequency (MF) = 4.28 + 1.34x + 7,51x(2) for Cs-137 (R-2 = 0.95) and MF = 4.81 + 0.67x for Rn-222 (R-2 = 0.5 1). post Cs-137 irradiation incubation in the presence of cytosine arabinoside, a reversible inhibitor of DNA repair, caused an increase in the MF over irradiation alone, consistent with a misrepair mechanism being involved in the mutagenicity of low-LET irradiation. The spectrum of Cs-137 irradiation-induced mutation displayed an increase in macro-deletions (in particular total gene deletions) and rearrangement events, some of which were further defined by either chromosome painting or direct DNA sequencing. The spectrum of Rn-222 irradiation-induced mutation was characterized by an increase in small alterations, especially multiple single base deletions/substitutions and micro-deletions. These studies define the specific response of human peripheral blood T cells to ionizing irradiation in vitro and form a basis for evaluating the genotoxic effects of human in vivo exposure.
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