TY - JOUR AB - Maternal embryonic leucine zipper kinase (MELK) has been reported to serve critical roles in the maintenance of stemness of cancer cells, although its mechanism remains unclear. Since SRY‑box 2 (SOX2) was demonstrated to be involved in self‑renewal and tumorigenicity of head and neck squamous cell carcinoma (HNSCC) and is aberrantly expressed in HNSCC tumors, the association between MELK and SOX2 was examined. Firstly, MELK inhibition was performed by small interfering RNA or MELK inhibitor OTS167, and it was determined that MELK inhibition by these approaches could decrease the SOX2 expression in HNSCC cells and OTS167 could suppress the SOX2 expression in a dose‑dependent manner. The present results indicated that MELK inhibition may target cancer stem cells (CSCs) through downregulation of the SOX2 gene. To further confirm the transcriptional regulation of SOX2, the transcription factors (TFs) were screened for SOX2 using a promoter‑binding TF assay followed by reverse transcription‑quantitative polymerase chain reaction and a decrease of the majority of the SOX2 TFs following MELK knockdown was observed. The present results provide evidence that MELK serves a key role in CSCs through the regulation of SOX2 and further indicates that MELK inhibition may also be promising for clinical applications in the treatment of HNSCC. AD - Department of Medicine, The University of Chicago, Chicago, IL 60637, USA AU - Ren,Lili AU - Deng,Boya AU - Saloura,Vassiliki AU - Park,Jae‑Hyun AU - Nakamura,Yusuke DA - 2019/04/01 DO - 10.3892/or.2019.6988 EP - 2548 IS - 4 JO - Oncol Rep KW - cancer stem cell kinase inhibitors head and neck cancer MELK SRY‑box 2 PY - 2019 SN - 1021-335X 1791-2431 SP - 2540 ST - MELK inhibition targets cancer stem cells through downregulation of SOX2 expression in head and neck cancer cells T2 - Oncology Reports TI - MELK inhibition targets cancer stem cells through downregulation of SOX2 expression in head and neck cancer cells UR - https://doi.org/10.3892/or.2019.6988 VL - 41 ER -