RANK Ligand Modulation of Autophagy in Oral Squamous Cell Carcinoma Tumor Cells

ABSTRACT Autophagy is a cellular process to recycle nutrients and has been implicated in cancer treatment. Oral squamous cell carcinoma (OSCC) is the most common oral cancer which ranks 3% of cancers in men and 2% in women. In this study, immunohistochemical staining of OSCC tumor specimens from human subjects and an athymic mouse model demonstrated high levels of autophagy markers LC3‐II and ATG5 expression. Further, we identified high levels LC3‐II expression in OSCC tumor cell lines (SCC‐1, SCC‐12, and SCC‐14a) compared to normal human epithelial (RWPE‐1) cells. OSCC cells express high levels of RANK ligand (RANKL); however, a functional role in autophagy is unknown. Interestingly, RANKL stimulation significantly increased autophagosome‐related gene expressions such as LC3, ATG5, BECN1, and PI3KC3 mRNA expression in OSCC cells. Further, Western blot analysis of total cell lysates demonstrated a dose‐dependent increase in LC3‐II and ATG5 expression in RANKL‐stimulated cells. In addition, RANKL increased expression of LC3‐I and LC3‐II, essential for autophagosome formation. Confocal microscopy analysis of LC3‐II and localization with lysosome further confirms autophagosome formation in response to RANKL treatment in OSCC cells. Collectively, our results indicate a novel function of RANKL to induce autophagosome formation, and could be a potential therapeutic target to control OSCC tumor progression. J. Cell. Biochem. 117: 118–125, 2016. © 2015 Wiley Periodicals, Inc.