SDCBP Modulates Stemness and Chemoresistance in Head and Neck Squamous Cell Carcinoma through Src Activation

Author:

Mir CristinaORCID,Garcia-Mayea YoelsisORCID,Garcia LaiaORCID,Herrero Pol,Canela NuriaORCID,Tabernero RocíoORCID,Lorente Juan,Castellvi JosepORCID,Allonca Eva,García-Pedrero Juana,Rodrigo Juan PabloORCID,Carracedo ÁngelORCID,LLeonart Matilde Esther

Abstract

To characterize the mechanisms that govern chemoresistance, we performed a comparative proteomic study analyzing head and neck squamous cell carcinoma (HNSCC) cells: CCL-138 (parental), CCL-138-R (cisplatin-resistant), and cancer stem cells (CSCs). Syntenin-1 (SDCBP) was upregulated in CCL-138-R cells and CSCs over parental cells. SDCBP depletion sensitized biopsy-derived and established HNSCC cell lines to cisplatin (CDDP) and reduced CSC markers, Src activation being the main SDCBP downstream target. In mice, SDCBP-depleted cells formed tumors with decreased mitosis, Ki-67 positivity, and metastasis over controls. Moreover, the fusocellular pattern of CCL-138-R cell-derived tumors reverted to a more epithelial morphology upon SDCBP silencing. Importantly, SDCBP expression was associated with Src activation, poor differentiated tumor grade, advanced tumor stage, and shorter survival rates in a series of 382 HNSCC patients. Our results reveal that SDCBP might be a promising therapeutic target for effectively eliminating CSCs and CDDP resistance.

Funder

Asociación Española Contra el Cáncer

Instituto de Salud Carlos III

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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