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Merck
  • CSPG4-specific immunity and survival prolongation in dogs with oral malignant melanoma immunized with human CSPG4 DNA.

CSPG4-specific immunity and survival prolongation in dogs with oral malignant melanoma immunized with human CSPG4 DNA.

Clinical cancer research : an official journal of the American Association for Cancer Research (2014-05-31)
Federica Riccardo, Selina Iussich, Lorella Maniscalco, Saray Lorda Mayayo, Giuseppe La Rosa, Maddalena Arigoni, Raffaella De Maria, Francesca Gattino, Stefania Lanzardo, Elena Lardone, Marina Martano, Emanuela Morello, Simone Prestigio, Alessandra Fiore, Elena Quaglino, Sara Zabarino, Soldano Ferrone, Paolo Buracco, Federica Cavallo
摘要

Due to the many similarities with its human counterpart, canine malignant melanoma (cMM) is a valuable model in which to assess the efficacy of novel therapeutic strategies. The model is herein used to evaluate the immunogenicity, safety, and therapeutic efficacy of a human chondroitin sulfate proteoglycan-4 (hCSPG4) DNA-based vaccine. The fact that homology between hCSPG4 and cCSPG4 amino-acidic sequences stands at more than 80% provides the rationale for using an hCSPG4 DNA vaccine in the cMM model. Dogs with stage II-III surgically resected CSPG4-positive oral MM were subjected to monthly intramuscular plasmid administration, which was followed immediately by electroporation (electrovaccination) for at least 6, and up to 20, months. The immunogenicity, safety, and therapeutic efficacy of the vaccine have been evaluated. hCSPG4 electrovaccination caused no clinically relevant local or systemic side effects and resulted in significantly longer overall and disease-free survival times in 14 vaccinated dogs as compared with 13 nonvaccinated controls. All vaccinated dogs developed antibodies against both hCSPG4 and cCSPG4. Seven vaccinated dogs were also tested for a cCSPG4-specific T-cell response and only two gave a detectable interferon (IFN)γ response. Xenogeneic electrovaccination against CSPG4 is able to overcome host unresponsiveness to the "self" antigen and seems to be effective in treating cMM, laying the foundation for its translation to a human clinical setting.

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Sigma-Aldrich
Anti-Dog IgG (whole molecule)–FITC antibody produced in rabbit, affinity isolated antibody, buffered aqueous solution