[No authors listed]
Remodeling and spacing factor 1 (Rsfâ1) has been reported as overexpressed in numerous cancers; however, its expression, biological functions and mechanisms in malignant melanoma remain unknown. In the present study, the expression of Rsfâ1 was investigated in 50 cases of malignant melanoma samples using immunohistochemistry. The results revealed that Rsfâ1 expression was elevated in 38% of specimens. MTT, colony formation, Transwell and flow cytometry assays were performed to investigate the functions of Rsfâ1. Knockdown of Rsfâ1 in the MV3 and A375 melanoma cell lines decreased the viability, invasion and cell cycle transition of cells. Conversely, overexpression of Rsfâ1 in M14 cells with low endogenous Rsfâ1 expression induced opposing effects. Further analysis revealed that Rsfâ1 knockdown decreased matrix metalloproteinaseâ2, cyclin E and phosphorylatedâIκB expression. Additionally, Rsfâ1 depletion reduced cisplatin resistance and significantly increased the cisplatinâassociated apoptotic rate, whereas Rsfâ1 overexpression exhibited opposing effects. Rsfâ1 also maintained the mitochondrial membrane potential following cisplatin treatment. Analysis of apoptosisâassociated proteins revealed that Rsfâ1 positively regulated Bâcell lymphoma 2 (Bclâ2), cellular inhibitor of apoptosis 1 (cIAP1) and cIAP2, and downregulated Bclâ2âassociated X protein expression. Nuclear factor κâlightâchainâenhancer of activated Bâcells (NFâκB) inhibition reversed the effects of Rsfâ1 on Bclâ2. In conclusion, Rsfâ1 was overexpressed in malignant melanoma and may contribute to the malignant behaviors of melanoma cells, possibly via the regulation of NFâκB signaling. Therefore, Rsfâ1 may be a potential therapeutic target in the treatment of malignant melanoma.
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