Abstract
BackgroundDevelopment of breast cancer is a multistage process influenced by hormonal and environmental factors as well as by genetic background. The search for genes underlying this malignancy has recently been highly productive, but the etiology behind this complex disease is still not understood. In studies using animal cancer models, heterogeneity of the genetic background and environmental factors is reduced and thus analysis and identification of genetic aberrations in tumors may become easier. To identify chromosomal regions potentially involved in the initiation and progression of mammary cancer, in the present work we subjected a subset of experimental mammary tumors to cytogenetic and molecular genetic analysis.MethodsMammary tumors were induced with DMBA (7,12-dimethylbenz[a]anthrazene) in female rats from the susceptible SPRD-Cu3 strain and from crosses and backcrosses between this strain and the resistant WKY strain. We first produced a general overview of chromosomal aberrations in the tumors using conventional kartyotyping (G-banding) and Comparative Genome Hybridization (CGH) analyses. Particular chromosomal changes were then analyzed in more details using an in-house developed BAC (bacterial artificial chromosome) CGH-array platform.ResultsTumors appeared to be diploid by conventional karyotyping, however several sub-microscopic chromosome gains or losses in the tumor material were identified by BAC CGH-array analysis. An oncogenetic tree analysis based on the BAC CGH-array data suggested gain of rat chromosome (RNO) band 12q11, loss of RNO5q32 or RNO6q21 as the earliest events in the development of these mammary tumors.ConclusionsSome of the identified changes appear to be more specific for DMBA-induced mammary tumors and some are similar to those previously reported in ACI rat model for estradiol-induced mammary tumors. The later group of changes is more interesting, since they may represent anomalies that involve genes with a critical role in mammary tumor development. Genetic changes identified in this work are at very small scales and thus may provide a more feasible basis for the identification of the target gene(s). Identification of the genes underlying these chromosome changes can provide new insights to the mechanisms of mammary carcinogenesis.
Highlights
Development of breast cancer is a multistage process influenced by hormonal and environmental factors as well as by genetic background
In the present work, SPRD-Cu3, F1-cross and backcrosses from SPRD-CU3 and Wistar Kyoto rats (WKY) strains were used to obtain a set of tumors with different genetic background
Three chromosomes, RNO10, RNO12 and RNO20, displayed moderate gains in more than 20% of the tumors (Figure 1), in those derived from the inbred SPRD-CU3 and the backcross animals (Additional file 1: Table S1)
Summary
Development of breast cancer is a multistage process influenced by hormonal and environmental factors as well as by genetic background. To identify chromosomal regions potentially involved in the initiation and progression of mammary cancer, in the present work we subjected a subset of experimental mammary tumors to cytogenetic and molecular genetic analysis. Genetic aberrations such as deletions and amplifications are known to be involved in tumor initiation and progression [1,2,3] and their analysis may provide valuable information about regions of the genome harboring cancer-related genes. The BAC (bacterial artificial chromosome) CGH-array technique uses a platform composed of genomic DNA fragments cloned in BAC clones This method provides a reasonably high resolution (hundreds kilobases, kb) and generates high signal to noise ratios [4,5]. The majority (over 70%) of the hereditary cases are thought to be caused by the interactions of multiple genes with low-penetrance and most of these genes remain to be identified
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