Human malignancies are often hallmarked with genomic instability, which itself is also considered a causative event in malignant transformation. Genomic instability may manifest itself as genetic changes in the nucleotide sequence of DNA, or as structural or numerical changes of chromosomes. Unrepaired or insufficiently repaired DNA double-strand breaks, as well as telomere shortening, are important contributors in the formation of structural chromosomal aberrations (CAs). In the present review, we discuss potential mechanisms behind the formation of CAs and their relation to cancer. Based on our own studies, we also illustrate how inherited genetic variation may modify the frequency and types of CAs occurring in humans. Recently, we published a series of studies on variations in genes relevant to maintaining genomic integrity, such as those encoding xenobiotic-metabolising enzymes, DNA repair, the tumour suppressor TP53, the spindle assembly checkpoint, and cyclin D1 (CCND1). While individually genetic variation in these genes exerted small modulating effects, in interactions they were associated with CA frequencies in peripheral blood lymphocytes of healthy volunteers. Moreover, we observed opposite associations between the CCND1 splice site polymorphism rs9344 G870A and the frequency of CAs compared to their association with translocation t(11,14). We discuss the functional consequences of the CCND1 gene in interplay with DNA damage response and DNA repair during malignant transformation. Our review summarizes existing evidence that gene variations in relevant cellular pathways modulate the frequency of CAs, predominantly in a complex interaction. More functional/mechanistic studies elucidating these observations are required. Several questions emerge, such as the role of CAs in malignancies with respect to a particular phenotype and heterogeneity, the formation of CAs during the process of malignant transformation, and the formation of CAs in individual types of lymphocytes in relation to the immune response.

Biomedical Center Martin Comenius University in Bratislava Jessenius Faculty of Medicine Martin 03601 Slovakia

Department of Medical Genetics 3rd Faculty of Medicine Charles University Prague 10000 Czech Republic

Department of Molecular Biology of Cancer Institute of Experimental Medicine Czech Academy of Sciences Prague 14220 Czech Republic; Faculty of Medicine and Biomedical Center in Pilsen Charles University Pilsen 30605 Czech Republic

Department of Molecular Biology of Cancer Institute of Experimental Medicine Czech Academy of Sciences Prague 14220 Czech Republic; Institute of Biology and Medical Genetics 1st Faculty of Medicine Charles University Prague 12800 Czech Republic; Department of Medical Genetics 3rd Faculty of Medicine Charles University Prague 10000 Czech Republic

Department of Molecular Biology of Cancer Institute of Experimental Medicine Czech Academy of Sciences Prague 14220 Czech Republic; Institute of Biology and Medical Genetics 1st Faculty of Medicine Charles University Prague 12800 Czech Republic; Faculty of Medicine and Biomedical Center in Pilsen Charles University Pilsen 30605 Czech Republic

Department of Molecular Biology of Cancer Institute of Experimental Medicine Czech Academy of Sciences Prague 14220 Czech Republic; Italian Institute for Genomic Medicine Torino 10126 Italy

Division of Molecular Genetic Epidemiology German Cancer Research Center Heidelberg D69120 Germany

Division of Molecular Genetic Epidemiology German Cancer Research Center Heidelberg D69120 Germany; Center for Primary Health Care Research Lund University Malmö 214 28 Sweden

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