Identification of microRNAs expression patterns in breast cancer in young women

A rise in the incidence of breast cancer among young adult women (with age 35) was observed in recent decades. Breast cancer incidence in young woman has been correlated to poor survival and aggressive features. Due to different type of breast cancers in young woman, 8- 10% with familial history appears with mutation in BRCA1/2 genes, and similar proportion occurs in cases without familial history (3- 10%). However, early onset breast cancer patients with or without familial history, non carriers of BRCA1/BRCA2 mutations is not well elucidated. The deregulation by microRNAs has recently emerged as a major determinant of tumorigenesis. Because miRNAs function by targeting functionally important protein-conding genes, it is of outstanding interest to identify miRNAs involved in the molecular mechanism underlying aggressiveness in tumors of young patients that might represent biomarkers and therapeutic targets. This evidence suggests that breast cancer in young woman has specific biological characteristics. Understanding the patterns of miRNAs expression that potentially alter the regulation of key breast cancer genes we could give a better treatment to these patients. Thirty-two patients were selected: 8 with familial history of breast and ovarian suggestive of hereditary condition according to NCCN criteria and 20 without familial history. Patients of both groups were of non carriers of BRCA1/BRCA2 mutations. The determination of microRNA expression network between those 2 groups was performed by TaqMan microRNA Assay (Applied Biosystems) using as control 3 normal mamoplastia samples from wealthy young women. Data were normalized using endogenous miRNA presented in each array. Statistical comparisons were done using ANOVA and Student T test with adjusted FDR (5%). It was found that 246 miRNAs were differently expressed between the 3 groups. From the comparison of familial group against normal group it was found 137 miRNAs differently expressed. In the comparison between non familial and normal group it was found 44 miRNAs differently expressed. Finally the comparison between familial group and non familial group it was found 4 miRNAs differently expressed. Among these miRNAs are some which was well characterized in breast cancer with down-regulation such as: miR-125b, miR-126 and miR-100. Our findings suggested that tumors from familial or sporadic cases presented discrete differences of microRNA expression patterns. A global downregulation of 137 miRNAs in tumors from familial group of patients when compared to normal group was observed. Based on the literature, most of these miRNAs are related to mechanisms of proliferation, cells migration and apoptosis. To our knowledge, this is the first evidence of miRNA expression in tumors of early onset Breast Cancer patients, non carries BRCA1/2 mutation, providing insights that may lead to the detection of new conducts of treatment (AU)