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MicroRNA-217 modulates pancreatic cancer progression via targeting ATAD2

Life Sci. 2022-04; 
Madhuri Dutta, Biswajit Das, Debasish Mohapatra, Padmanava Behera, Shantibhusan Senapati, Anasuya Roychowdhury
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Recombinant Proteins … -3′ UTR) was designed and purchased from GenScript. For the Dual-luciferase reporter assay… Higher expression of ATAD2 across the PCCs and PAAD tumor tissues encouraged us to … Get A Quote

摘要

objective: Pancreatic cancer is a fatal disease across the world with 5?years survival rate less than 10%. ATAD2, a valid cancer drug-target, is overexpressed in pancreatic malignancy with high oncogenic potential. However, the mechanism of the upregulated expression of ATAD2 in pancreatic cancer is unknown. Since microRNAs (miRNAs) could potentially control target mRNA expressions, and are involved in cancer as tumor-suppressors, oncomiR or both, we examine the possibility of miRNA-mediated regulation of ATAD2 in pancreatic cancer cells (PCCs). methods: Our in-silico approach first identifies hsa-miR-217 as a candidate regulator for ATAD2 expression. For further validation, luciferase reporter assay is perfor... More

關鍵詞

AKT pathway, ATAD2, Cell viability, Migration, Pancreatic ductal adenocarcinoma, hsa-miR-217
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