On the difference of micronucleus frequencies in peripheral blood lymphocytes between breast cancer patients and controls

doi:10.1093/mutage/gel035

Mutagenesis Advance Access originally published online on August 22, 2006
Mutagenesis 2006 21(5):313-320; doi:10.1093/mutage/gel035

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On the difference of micronucleus frequencies in peripheral blood lymphocytes between breast cancer patients and controls

Dominic Varga¹^,2, Josef Hoegel¹, Christiane Maier¹, Silke Jainta¹, Maren Hoehne¹, Brenda Patino-Garcia¹, Isabell Michel¹, Ulrike Schwarz-Boeger³, Marion Kiechle³, Rolf Kreienberg² and Walther Vogel¹^,*

¹ Department of Human Genetics, University of Ulm Germany ² Department of Gynecology, University of Ulm Germany ³ Department of Gynecology, Technische Universitaet Muenchen Germany

Sporadic breast cancer patients as well as mutation carriersof the BRCA genes have a reduced DNA repair capacity comparedto controls when assessed by the G₀ micronucleus test (G₀MNT)or by induced chromosomal aberrations. Since the individualMN frequencies vary widely and overlap between cases and controlsit remained unclear which percentage of the cases should beconsidered to exhibit an increased radiosensitivity. We performeda similar case–control study and found a highly significantdifference (P < 0.0001) between all breast cancer cases (N= 91) and female controls (N = 96) using descriptive statisticsand ANOVA with adjustment for age. This difference also holdsfor baseline MN frequencies (P = 0.0006) and for subgroups ofthe patients similar to those without treatment (P < 0.0001).These results were confirmed in a second sample acquired ata different hospital. Since we are dealing in this analysiswith two predefined groups (patients and controls), we calculatedodds ratios (ORs) in order to assess the discriminative powerof the G₀MNT. These amounted to OR = 4.9 (P < 0.0001) forMN frequencies obtained by visual counting and ranged from OR= 11 (P < 0.0011) to OR = 22 (P < 0.0001) using automatedcounting. In order to overcome the problem of choosing a cut-offpoint inherent in ORs, receiver operating characteristic curveswere calculated, which visualize specificity and sensitivityover the entire range of values and which characterize the discriminativepower of a test by the area under the curve (AUC) (visual counting,baseline: AUC = 0.67; induced AUC = 0.75; automated counting:AUC > 0.88; evaluation sample: AUC > 0.73). We concludethat the G₀MNT may be a useful tool to substitute the phenotypebreast cancer in association and linkage studies and that itmay be possible to develop a test useful in the diagnosis orrisk assessment for breast cancer.

^*To whom correspondence should be addressed at: Department of Human Genetics, University of Ulm, 89069 Ulm, Germany. Tel: +49 731 50023430; Fax: +49 731 50023438; Email: walther.vogel{at}uni-ulm.de

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