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Review article

Survivin-Based Treatment Strategies for Squamous Cell Carcinoma

Andrea SantarelliDentistry Clinic, National Institute of Health and Science of Aging, INRCA, 60126 Ancona, ItalyMarco MascittiDepartment of Clinical Specialistic and Dental Sciences, Marche Polytechnic University, Via Tronto 10, 60126 Ancona, ItalyLucio Lo RussoDepartment of Clinical and Experimental Medicine, Foggia University, Via Rovelli 50, 71122 Foggia, ItalyDavide SartiniDepartment of Clinical Specialistic and Dental Sciences, Marche Polytechnic University, Via Tronto 10, 60126 Ancona, ItalyGiuseppe TroianoDepartment of Clinical and Experimental Medicine, Foggia University, Via Rovelli 50, 71122 Foggia, ItalyMonica EmanuelliDepartment of Clinical Specialistic and Dental Sciences, Marche Polytechnic University, Via Tronto 10, 60126 Ancona, ItalyLorenzo Lo MuzioDepartment of Clinical and Experimental Medicine, Foggia University, Via Rovelli 50, 71122 Foggia, Italy
2018en
ABI

Abstract

Survivin, an anti-apoptotic molecule abundantly expressed in most human neoplasms, has been reported to contribute to cancer initiation and drug resistance in a wide variety of human tumors. Efficient downregulation of survivin can sensitize tumor cells to various therapeutic interventions, generating considerable efforts in its validation as a new target in cancer therapy. This review thoroughly analyzes up-to-date information on the potential of survivin as a therapeutic target for new anticancer treatments. The literature dealing with the therapeutic targeting of survivin will be reviewed, discussing specifically squamous cell carcinomas (SCCs), and with emphasis on the last clinical trials. This review gives insight into the recent developments undertaken in validating various treatment strategies that target survivin in SCCs and analyze the translational possibility, identifying those strategies that seem to be the closest to being incorporated into clinical practice. The most recent developments, such as dominant-negative survivin mutants, RNA interference, anti-sense oligonucleotides, small-molecule inhibitors, and peptide-based immunotherapy, seem to be helpful for effectively downregulating survivin expression and reducing tumor growth potential, increasing the apoptotic rate, and sensitizing tumor cells to chemo- and radiotherapy. However, selective and efficient targeting of survivin in clinical trials still poses a major challenge.

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