Abstract
BackgroundMicroRNAs may act as oncogenes or tumour suppressor genes, which make these small molecules potential diagnostic/prognostic factors and targets for anticancer therapies. Several common oncogenic microRNAs have been found for canine mammary cancer and human breast cancer. On account of this, large-scale profiling of microRNA expression in canine mammary cancer seems to be important for both dogs and humans.MethodsExpression profiles of 317 microRNAs in 146 canine mammary tumours of different histological type, malignancy grade and clinical history (presence/absence of metastases) and in 25 control samples were evaluated. The profiling was performed using microarrays. Significance Analysis of Microarrays test was applied in the analysis of microarray data (both unsupervised and supervised data analyses were performed). Validation of the obtained results was performed using real-time qPCR. Subsequently, predicted targets for the microRNAs were searched for in miRBase.ResultsResults of the unsupervised analysis indicate that the primary factor separating the samples is the metastasis status. Predicted targets for microRNAs differentially expressed in the metastatic vs. non-metastatic group are mostly engaged in cell cycle regulation, cell differentiation and DNA-damage repair. On the other hand, the supervised analysis reveals clusters of differentially expressed microRNAs unique for the tumour type, malignancy grade and metastasis factor.ConclusionsThe most significant difference in microRNA expression was observed between the metastatic and non-metastatic group, which suggests a more important role of microRNAs in the metastasis process than in the malignant transformation. Moreover, the differentially expressed microRNAs constitute potential metastasis markers. However, validation of cfa-miR-144, cfa-miR-32 and cfa-miR-374a levels in blood samples did not follow changes observed in the non-metastatic and metastatic tumours.
Highlights
MicroRNAs may act as oncogenes or tumour suppressor genes, which make these small molecules potential diagnostic/prognostic factors and targets for anticancer therapies
MicroRNA microarray analysis The technical data quality assessment showed that the sample labelling with Hy3TM and Hy5TM fluorescent labels was successful as all capture probes for the control spike-in oligonucleotides produced signals in the expected range
We searched in miRBase [29] for predicted targets of microRNAs that we found differentially expressed in metastatic when compared to non-metastatic canine mammary cancer
Summary
MicroRNAs may act as oncogenes or tumour suppressor genes, which make these small molecules potential diagnostic/prognostic factors and targets for anticancer therapies. Several common oncogenic microRNAs have been found for canine mammary cancer and human breast cancer. Mammary tumours occur spontaneously in dog and human populations [1]. Many similar oncogenes were found for human breast cancer and canine mammary carcinoma, for instance oncogenic microRNAs [9]. Many changes in pathways related to mammary cancer (including KRAS, PTEN, PI3K/AKT, WNT-beta catenin and MAPK cascade) are common for both species [10]. All these molecular similarities made canine mammary cancer a good genetic model for human breast cancer [11]
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