Molecular characterisation of murine acute myeloid leukaemia induced by 56Fe ion and 137Cs gamma ray irradiation

Exposure to sparsely ionising gamma- or X-ray irradiation is known to increase the risk of leukaemia in humans. However, heavy ion radiotherapy and extended space exploration will expose humans to densely ionising high linear energy transfer (LET) radiation for which there is currently no understand...

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Published inMutagenesis Vol. 28; no. 1; pp. 71 - 79
Main Authors Steffen, Leta S, Bacher, Jeffery W, Peng, Yuanlin, Le, Phuong N, Ding, Liang-Hao, Genik, Paula C, Ray, F Andrew, Bedford, Joel S, Fallgren, Christina M, Bailey, Susan M, Ullrich, Robert L, Weil, Michael M, Story, Michael D
Format Journal Article
LanguageEnglish
Published England Oxford University Press 01.01.2013
Subjects
Animals
Cesium Radioisotopes
Chromatids - radiation effects
Chromosome Aberrations
Dose-Response Relationship, Radiation
Gamma Rays - adverse effects
In Situ Hybridization, Fluorescence
Iron
Leukemia, Myeloid, Acute - etiology
Leukemia, Myeloid, Acute - genetics
Leukemia, Radiation-Induced - genetics
Linear Energy Transfer
Male
Mice
Mice, Inbred CBA
Microsatellite Instability
Mutation
Original Manuscript
Proto-Oncogene Proteins - genetics
Single-Cell Analysis
Trans-Activators - genetics
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Summary:Exposure to sparsely ionising gamma- or X-ray irradiation is known to increase the risk of leukaemia in humans. However, heavy ion radiotherapy and extended space exploration will expose humans to densely ionising high linear energy transfer (LET) radiation for which there is currently no understanding of leukaemia risk. Murine models have implicated chromosomal deletion that includes the hematopoietic transcription factor gene, PU.1 (Sfpi1), and point mutation of the second PU.1 allele as the primary cause of low-LET radiation-induced murine acute myeloid leukaemia (rAML). Using array comparative genomic hybridisation, fluorescence in situ hybridisation and high resolution melt analysis, we have confirmed that biallelic PU.1 mutations are common in low-LET rAML, occurring in 88% of samples. Biallelic PU.1 mutations were also detected in the majority of high-LET rAML samples. Microsatellite instability was identified in 42% of all rAML samples, and 89% of samples carried increased microsatellite mutant frequencies at the single-cell level, indicative of ongoing instability. Instability was also observed cytogenetically as a 2-fold increase in chromatid-type aberrations. These data highlight the similarities in molecular characteristics of high-LET and low-LET rAML and confirm the presence of ongoing chromosomal and microsatellite instability in murine rAML.
ISSN:0267-8357
1464-3804
DOI:10.1093/mutage/ges055