Kaboudan F, Talesh Sasani S, Asghari S M. The effect of a VEGFB antagonist peptide on the expression level of miR-210 in a mouse model of breast cancer. nbr 2021; 8 (1) :13-19
URL:
http://nbr.khu.ac.ir/article-1-3376-en.html
Department of Biology, Faculty of Sciences, University of Guilan, Rasht, Iran , sasani@guilan.ac.ir
Abstract: (3252 Views)
Breast cancer is the fourth common cancer worldwide and occurs when breast cells begin to uncontrolled division and tumor formation. Angiogenesis is one of the essential factors in cell growth and maintenance of homeostasis in the natural and pathological conditions, while VEGFs are the most critical factors in angiogenesis. MiR-210 plays an important role in the angiogenesis via association with VEGF. Here, the miR-210 expression changes in response to a VEGFB antagonist peptide, called VEGB1, was studied in female BALB/c mice bearing 4T1 cell line induced breast tumor. The treated group received 1mg.kg-1 and 10mg.kg-1 of the peptide and the control group received PBS intraperitoneally during two weeks. Both of the animal groups underwent a resection of breast tissue 14 days after treatment and miR-210 expression level was investigated. Statistical analysis by On-way ANOVA showed that the expression level of miR-210 gene had significant differences among the groups treated with various doses of VEGB1. Also, the gene expression was significantly different between peptide-treated groups and control samples (p<0.05). MiR-210 expression level had 42% reduction in mice treated with 1mg.kg-1 of VEGB1, while 90% was seen in mice treated with 10mg.kg-1 of VEGB1 showing the inhibitory function of VEGB1 antagonist peptide at different doses.
Type of Study:
Original Article |
Subject:
Genetics Received: 2020/07/1 | Revised: 2021/06/4 | Accepted: 2020/10/28 | Published: 2021/06/5 | ePublished: 2021/06/5