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   An Integrative Analysis of the Micro-Rnas Contributing in Stemness, Metastasis and B-Raf Pathways in Malignant Melanoma and Melanoma Stem Cell  
   
نویسنده Sahranavardfard Parisa ,Madjd Zahra ,Emami Razavi Amirnader ,Ghanadan Alireza ,Firouzi Javad ,Khosravani Pardis ,Ghavami Saeid ,Ebrahimie Esmaeil ,Ebrahimi Marzieh
منبع Cell Journal (Yakhteh) - 2021 - دوره : 23 - شماره : 3 - صفحه:261 -272
چکیده    Objective: epithelial-mesenchymal transition (emt) and the stemness potency in association with braf mutation are in dispensable to the progression of melanoma. recently, micrornas (mirnas) have been introduced as the regulator of a multitude of oncogenic functions in most of tumors. therefore identifying and interpreting the expression patterns of these mirnas is essential. the present study sought to find common mirnas regulating all three important pathways in melanoma development. materials and methods: in this experimental study, 18 mirnas that importantly contribute to emt and have a role in regulating self-renewal and the braf pathway were selected based on current literature and cross-analysis with available databases. subsequently, their expression patterns were evaluated in 20 melanoma patients, normal tissues, serum from patients and control subjects, and melanospheres. pattern discovery and integrative regulatory network analysis were used to find the most important mirnas in melanoma progression. results: among 18 selected mirnas, mir-205, -141, -203, -15b, and -9 were differentially expressed in tumor samples than normal tissues. among them, mir-205, -15b, and -9 significantly expressed in serum samples and healthy donors. attribute weighting and decision trees (dt) analysis presented evidence that the combination of mir-205, -203, -9, and -15b can regulate self-renewal and emt process, by affecting cdh1, ccnd1, and vegf expression. conclusion: we suggested here that mir-205, -15b, -203, -9 pattern as the key mirnas linked to melanoma status, the pluripotency, proliferation, and motility of malignant cells. however, further investigations are required to find the mechanisms underlying the combinatory effects of the above mentioned mirnas.
کلیدواژه Epithelial-Mesenchymal Transition ,Melanoma ,Microrna ,Network Analysis
آدرس Academic Center For Education, Culture & Research (Acecr), Cell Science Research Center, Royan Institute For Stem Cell Biology And Technology, Department Of Stem Cells And Developmental Biology, Iran, Iran University Of Medical Sciences, Department Of Pathology, Iran, Tehran University Of Medical Sciences, Iran National Tumor Bank, Cancer Institute Of Iran, Iran, Tehran University Of Medical Sciences, Iran National Tumor Bank, Cancer Institute Of Iran, Razi Skin Hospital, Department Of Dermatopathology, Iran, Academic Center For Education, Culture & Research (Acecr), Cell Science Research Center, Royan Institute For Stem Cell Biology And Technology, Department Of Stem Cells And Developmental Biology, Iran, Academic Center For Education, Culture & Research (Acecr), Cell Science Research Center, Royan Institute For Stem Cell Biology And Technology, Department Of Stem Cells And Developmental Biology, Iran, University Of Manitoba, Biology Of Breathing, Children Hospital Research Institute, Research Institute In Oncology And Hematology, Cancer Care Manitoba, Department Of Human Anatomy And Cell Sciences, Canada. Shiraz University Of Medical Sciences, Autophagy Research Center, Iran, University Of Adelaide, School Of Animal And Veterinary Sciences, Australia. La Trobe University, School Of Life Sciences, College Of Science, Health And Engineering, Australia, Academic Center For Education, Culture And Research (Acecr), Cell Science Research Center, Royan Institute For Stem Cell Biology And Technology, Department Of Stem Cells And Developmental Biology, Iran
پست الکترونیکی esmaeil.ebrahimie@adelaide.edu.au; mebrahimi@royaninstitute.org
 
     
   
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