mFISH analysis of chromosome aberrations in workers occupationally exposed to mixed radiation

Sotnik, N.V.; Osovets, S. V.; Scherthan, Harry; Azizova, Tamara V.

doi:10.1007/s00411-014-0536-7

Cited by 23 publications

(16 citation statements)

References 51 publications

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“…The biological reason for this long-term survival of such heavily damaged PBLs is unclear. However, similar observations, at varying frequencies, have been reported elsewhere including in plutonium workers [87][88][89][90], thorotrast patients [85,91], veterans of nuclear testing [92], A-bomb survivors [93], astronauts and patients receiving carbon therapy [81]. Interestingly, Hande et al [79] found a significant correlation with estimated plutonium dose to the bone marrow (from ~500mGy) and yield of complex aberrations suggesting quantification could potentially be used for dose reconstruction.…”

Section: Complexity Per Se As An Indicator Of High-let Radiationsupporting

confidence: 65%

Cytogenetic Biomarkers of Radiation Exposure

Anderson

2019

Clinical Oncology

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Section: Complexity Per Se As An Indicator Of High-let Radiationsupporting

confidence: 65%

Cytogenetic Biomarkers of Radiation Exposure

Anderson

2019

Clinical Oncology

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“…Support for this comes from the in vitro work on long-term cultures reported here. Nevertheless, stable cells containing multiple aberrations are induced by a-particle radiation, albeit in small numbers, and have been observed in studies of workers exposed to internally deposited plutonium (Tawn et al 1985;Whitehouse et al 1998;Anderson et al 2005;Hande et al 2005;Livingston et al 2006;Tawn et al 2006;Sotnik et al 2014). In the current study, such cells were found in three of the nine men (Table 3).…”

Section: Discussionmentioning

confidence: 93%

“…A number of studies have characterized the chromosome aberrations observed in peripheral blood lymphocytes from nuclear workers exposed to a-particle-emitting internally deposited plutonium and attempted to relate these to the cumulative internal dose to the bone marrow (Brandom et al 1979;Tawn et al 1985;Brandom et al 1990;Whitehouse et al 1998;Hande et al 2003;Mitchell et al 2004;Anderson et al 2005;Hande et al 2005;Tawn and Whitehouse 2005;Livingston et al 2006;Tawn et al 2006;Sotnik et al 2014). The majority have identified translocations as the predominant aberration but, although their frequency is greater than that expected from any associated external low LET c-ray exposure, little has been achieved in terms of using translocation frequency to quantify the response following in vivo a-particle exposure.…”

Section: Introductionmentioning

confidence: 98%

Chromosome aberrations in workers with exposure to α-particle radiation from internal deposits of plutonium: expectations from in vitro studies and comparisons with workers with predominantly external γ-radiation exposure

Sotnik

et al. 2015

Radiat Environ Biophys

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mFISH analysis of chromosome aberration profiles of 47 and 144 h lymphocyte cultures following exposure to 193 mGy α-particle radiation confirmed that the frequency of stable aberrant cells and stable cells carrying translocations remains constant through repeated cell divisions. Age-specific rates and in vitro dose-response curves were used to derive expected translocation yields in nine workers from the Mayak nuclear facility in Russia. Five had external exposure to γ-radiation, two of whom also had exposure to neutrons, and four had external exposure to γ-radiation and internal exposure to α-particle radiation from incorporated plutonium. Doubts over the appropriateness of the dose response used to estimate translocations from the neutron component made interpretation difficult in two of the workers with external exposure, but the other three had translocation yields broadly in line with expectations. Three of the four plutonium workers had translocation yields in line with expectations, thus supporting the application of the recently derived in vitro α-particle dose response for translocations in stable cells. Overall this report demonstrates that with adequate reference in vitro dose-response curves, translocation yield has the potential to be a useful tool in the validation of red bone marrow doses resulting from mixed exposure to external and internal radiation.

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“…Non-targeted approaches such as metabolomics, lipidomics and proteomics have provided promising preliminary results for new biomarkers of exposure to radionuclides, as demonstrated by recent studies of uranium (lowest estimated calculated dose of 0.15 mGy in the kidney), 137 Cs (lowest average cumulated dose of 4mGy) and 90 Sr (lowest average cumulated dose of 1 Gy) contamination in rats [216,217,[265][266][267]. Translocations, complex chromosomal rearrangements and micronuclei in peripheral blood lymphocytes (see above) are also potentially useful to estimate cumulated red bone marrow doses resulting from protracted mixed exposure to internal and external IR following moderate to high doses, although further work is needed for complete validation [12,56,59,60,268]. Gender specific mRNA and miRNA gene expression patterns to internal 239 Pu exposure have been deciphered in former Mayak workers [269,270], which are promising markers of internal alpha-particle exposure and warrant further validation.…”

Section: New Biomarkers Of Exposure To Internal Emittersmentioning

confidence: 99%

Ionizing radiation biomarkers in epidemiological studies – An update

Hall

Jeggo

West

et al. 2017

Mutation Research/Reviews in Mutation Research

128

105

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Recent epidemiology studies highlighted the detrimental health effects of exposure to low dose and low dose rate ionizing radiation (IR): nuclear industry workers studies have shown increased leukaemia and solid tumour risks following cumulative doses of <100mSv and dose rates of <10mGy per year; paediatric patients studies have reported increased leukaemia and brain tumours risks after doses of 30-60mGy from computed tomography scans. Questions arise, however, about the impact of even lower doses and dose rates where classical epidemiological studies have limited power but where subsets within the large cohorts are expected to have an increased risk. Further progress requires integration of biomarkers or bioassays of individual exposure, effects and susceptibility to IR. The European DoReMi (Low Dose Research towards Multidisciplinary Integration) consortium previously reviewed biomarkers for potential use in IR epidemiological studies. Given the increased mechanistic understanding of responses to low dose radiation the current review provides an update covering technical advances and recent studies. A key issue identified is deciding which biomarkers to progress. A roadmap is provided for biomarker development from discovery to implementation and used to summarise the current status of proposed biomarkers for epidemiological studies. Most potential biomarkers remain at the discovery stage and for some there is sufficient evidence that further development is not warranted. One biomarker identified in the final stages of development and as a priority for further research is radiation specific mRNA transcript profiles.

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mFISH analysis of chromosome aberrations in workers occupationally exposed to mixed radiation

Cited by 23 publications

References 51 publications

Cytogenetic Biomarkers of Radiation Exposure

Cytogenetic Biomarkers of Radiation Exposure

Chromosome aberrations in workers with exposure to α-particle radiation from internal deposits of plutonium: expectations from in vitro studies and comparisons with workers with predominantly external γ-radiation exposure

Ionizing radiation biomarkers in epidemiological studies – An update

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