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Vaccination with human tyrosinase DNA induces antibody responses in dogs with advanced melanoma.


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.

SUBMITTER: Liao JC 

PROVIDER: S-EPMC1976276 | biostudies-literature | 2006 Apr

REPOSITORIES: biostudies-literature

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Vaccination with human tyrosinase DNA induces antibody responses in dogs with advanced melanoma.

Liao Jack C F JC   Gregor Polly P   Wolchok Jedd D JD   Orlandi Francesca F   Craft Diane D   Leung Carrie C   Houghton Alan N AN   Bergman Philip J PJ  

Cancer immunity 20060421


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-m  ...[more]

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