4.5 Review

Synovial sarcoma is a gateway to the role of chromatin remodeling in cancer

Journal

CANCER AND METASTASIS REVIEWS
Volume 34, Issue 3, Pages 417-428

Publisher

SPRINGER
DOI: 10.1007/s10555-015-9575-z

Keywords

Synovial sarcoma; SS18-SSX; Fusion protein; Protein interaction; SWI/SNF; Targeted therapy

Categories

Funding

  1. Children's Cancer Foundation, Baltimore, MD
  2. St. Baldrick's Foundation
  3. Burroughs Wellcome Clinical Scientist Award in Translational Research
  4. Mildred-Scheel-Postdoktoranden-Programm of Deutsche Krebshilfe
  5. NIH [R01CA133662, R01CA138212]

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Patients afflicted with synovial sarcoma share the fate of other translocation positive sarcomas; the driver mutation for this cancer is known, yet no means to target the fusion protein SS18-SSX directly exist. Current chemotherapeutic regimens are minimally beneficial, particularly in patients with metastatic disease. SS18-SSX putatively promotes its oncogenic activity through protein-protein interactions that alter genetic programs through chromatin remodeling. This review discusses the functional protein network of SS18-SSX, both wild-type and fusion protein, considers its intrinsically disordered nature, and provides insights into potential therapeutic strategies. A comprehensive overview of the clinical characteristics reveals the need for newly targeted therapeutics based upon oncogenic transformation by the fusion protein SS18-SSX. The wild-type, non-fused proteins SS18 and SSX are presented including their molecular structure and biological function with regard to protein-protein interactions. The interactions of the wild-type proteins inform the oncogenic changes of the fusion protein. The SS18-SSX fusion protein and its protein interactions are described and evaluated for their biological consequences that lead to oncogenesis. This review illustrates the key protein interactions of SS18-SSX that may qualify as primary targets for small molecule-based disruption leading to the development of SS18-SSX-specific drugs. These novel targeted therapeutics may provide a specificity that ultimately improves survival while reducing morbidity of patients with synovial sarcoma.

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