Publication | Open Access
MiR-381-3p suppresses biological characteristics of cancer in head-neck squamous cell carcinoma cells by targeting nuclear autoantigenic sperm protein (NASP)
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Citations
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References
2019
Year
Cancer BiologyEpigeneticsTumor BiologyTranscriptional RegulationCancer Cell BiologyNasp GeneRadiation OncologyCancer ResearchWhether NaspCell LinesGene ExpressionEpigenetic RegulationCell BiologyMicrorna DetectionTumor MicroenvironmentChromatinNatural SciencesSmall RnaTumor SuppressorMedicineCell DevelopmentNon-coding Rna
MiR-381-3p and nuclear autoantigenic sperm protein (NASP) have regulatory functions in tumors. Whether NASP is targeted by miR-381-3p to influence biological characteristics of cancer in head-neck squamous cell carcinoma (HNSCC) cells was investigated. StarBase (version 3.0) found that the expression of NASP was increased with the down-regulation of miR-381-3p in laryngocarcinoma tissue, AMC-HN-3,FaDu,HNE-3,and Detroit 562 cell lines. MiR-381-3p could target NASP, reduce the expression of MMP-2 and MMP-9, Vimentin, repress the cell viability, invasion, and migration, and promote the expression of E-cadherin in AMC-HN-3 cells. Overexpressed NASP could increase the viability, migration and invasion rates in AMC-HN-3 cells, which could be partially reversed by overexpressed miR-381-3p. Thus, miR-381-3p targeted and suppressed NASP gene, reduced the viability, migration, invasion, EMT of HNSCC cells, demonstrating that miR-381-3p has the potential to be a therapeutic target in inhibiting the progression of HNSCC.
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