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Genome Damage in Oropharyngeal Cancer Patients Treated by Radiotherapy

Marija Gamulin ; Department of Oncology, Zagreb University Hospital Center, Zagreb, Croatia
Nevenka Kopjar ; Institute for Medical Research and Occupational Health Mutagenesis Unit, Zagreb, Croatia
Mislav Grgić ; Department of Oncology, Zagreb University Hospital Center, Zagreb, Croatia
Snježana Ramić ; The University Hospital for Tumors, Zagreb, Croatia
Vesna Bišof ; Department of Oncology, Zagreb University Hospital Center, Zagreb, Croatia
Vera Garaj-Vrhovac ; Institute for Medical Research and Occupational Health Mutagenesis Unit, Zagreb, Croatia


Puni tekst: engleski pdf 539 Kb

str. 515-527

preuzimanja: 487

citiraj


Sažetak

Aim To estimate genome damage in oropharyngeal cancer patients before, during, and after radiotherapy and to measure the persistence of caused genome damage relevant in the evaluation of secondary cancer risk. Methods DNA damage was evaluated in peripheral blood lymphocytes of 10 oropharyngeal cancer patients using alkaline comet assay, analysis of structural chromosome aberrations, and micronucleus assay. Blood samples were taken 2 hours before irradiation on day 1 of the first radiotherapy
cycle, 2 hours after the application of the first dose, in the
middle of the radiotherapy cycle, within 2 hours after the last received
radiotherapy dose, and after 6 and 12 months after radiotherapy.
Results In most participants, the highest level of primary DNA damage was recorded in blood samples collected after the administration of first radiation dose (mean tail length 25.04 ± 6.23 μm). Most patients also had increased frequency of comets with long tail-nucleus (LTN comets) after the administration of the first radiation dose (mean, 10.50 ± 7.71 per 100 comets), which remained increased in the middle of radiotherapy (mean, 18.30 ± 27.62 per 100 comets). Later on, the levels of primary DNA damage
as recorded by the comet assay, slightly diminished. The frequency of
structural chromosome aberrations in lymphocytes gradually increased during the radiation cycle (26.50 ± 27.72 per 100 metaphases at the end of the therapy), as well as the frequency of micronuclei (mean total number of micronuclei 167.20 ± 35.69 per 1000 binuclear cells). Conclusion Oropharyngeal cancer patients had relatively high levels of primary DNA damage in their peripheral blood lymphocytes even before therapy. The frequency of complex structural chromosome aberrations and the frequency of micronuclei increased with the progression of the radiation cycle and the doses delivered. As the frequency of chromosomal aberrations a year after radiotherapy mostly did not return to pre-therapy values, it represents an important risk factor related to the onset of second
cancer.

Ključne riječi

oropharyngeal cancer; genome damage; chromosome aberrations; micronucleus assay; comet assay

Hrčak ID:

29265

URI

https://hrcak.srce.hr/29265

Datum izdavanja:

15.8.2008.

Posjeta: 992 *