AI Article Synopsis

  • Researchers used plasmid DNA vaccines targeting specific cancer markers (melanosomal differentiation antigens) to stimulate immune responses against melanoma in mice, leading to the exploration of this approach in dogs.
  • In a Phase I clinical trial, nine dogs with advanced melanoma received a human tyrosinase DNA vaccine, showing safety and a longer survival compared to historical controls.
  • Three dogs developed antibodies specific to tyrosinase, indicating the vaccine's potential to overcome the dog's immune tolerance to its own proteins, which may correlate with their improved tumor control and survival rates.

Article Abstract

Antitumor immune responses can be elicited in preclinical mouse melanoma models using plasmid DNA vaccines encoding xenogeneic melanosomal differentiation antigens. We previously reported on a phase I clinical trial of human tyrosinase (huTyr) DNA vaccination of 9 dogs with advanced malignant melanoma (World Health Organization stages II-IV), in which we demonstrated the safety of the treatment and the prolongation of the expected survival time (ST) of subjects as compared to historical, stage-matched controls. As a secondary goal of the same study, we report here on the induction of tyrosinase-specific antibody responses in three of the nine dogs vaccinated with huTyr DNA. The antibodies in two of the three responders cross-react with syngeneic canine tyrosinase, demonstrating the ability of this vaccine to overcome host immune tolerance and/or ignorance to or of "self" antigens. Most interestingly, the onset of antibody induction in these three dogs coincides with observed clinical responses and may suggest a means to account for their long-term tumor control and survival.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1976276PMC

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