[No authors listed]
MicroRNAs (miRs) serve important roles in the formation and progression of papillary thyroid cancer (PTC) by regulating numerous physiological and pathological behaviours. Thus, investigating the functional roles of specific miRNAs in PTC may contribute in identifying effective therapeutic targets for the management of patients with PTC. miRâ744 is emerging as a cancerâassociated miRNA in numerous types of human cancers; however, the expression and specific functions of miRâ744 in PTC are yet to be determined, and the mechanism underlying the regulatory roles of miRâ744 in PTC remains unknown. In the present study, miRâ744 expression was significantly decreased in PTC tissues and cell lines, as detected by reverse transcriptionâquantitative polymerase chain reaction. miRâ744 restoration inhibited cell proliferation and invasion in PTC. Bioinformatics analysis predicted NIN1 (RPN12) binding protein 1 homolog (NOB1) as a potential target of miRâ744. Subsequent experiments validated NOB1 as a direct target gene of miRâ744 in PTC. Furthermore, NOB1 was upregulated in PTC tissues and negatively correlated with miRâ744 expression. NOB1 overexpression could counteract miRâ744âmediated antitumor effects on PTC cells. In summary, these findings indicated that miRâ744 may inhibit the progression of PTC by directly targeting NOB1. The identification of the miRâ744/NOB1 axis may provide insight into potential targets for the treatment of patients with PTC and improve their prognosis.
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