Background and aims: A GnRH-based, therapeutic vaccine candidate against hormone-sensitive prostate cancer has demonstrated its capacity to control the disease in phase I/II trials. Here, we characterized the isotype/subclass profiles of the anti-GnRH humoral response generated by the vaccination and analyzed it association with patients’ clinical outcomes.  Methods: The immunoglobulin isotypes and IgG subclass of the humoral immune response of 37 patients with locally advanced prostate adenocarcinoma, stages 3-4, immunized with the vaccine candidate, were characterized. Additionally, serum testosterone and PSA concentrations, as indicators of tumor response, were determined.

Results: All the patients developed strong and prolonged anti-GnRH antibody responses, which caused a short to mid-term decrease in serum levels of testosterone and PSA. After immunizations, anti-GnRH IgM/IgG and IgG1/IgG3 responses were found. Following radiotherapy, the humoral response switched to IgG (IgG1/IgG4). The patients who underwent a short-term biochemical relapse were characterized by significantly higher levels of anti-GnRH IgG titers, subclasses IgG1 and IgG4. The same characteristics, along with a high response of specific IgM antibodies at the end of immunizations, and the development of anti-GnRH IgA antibody responses following radiotherapy, were observed in patients whose disease progressed, compared to the ones with the controlled disease. Conclusion: The type of the humoral response against anti-GnRH, induced by vaccination could be determinant to trigger other immunological mechanisms which, as a whole, contribute to the control of tumor growth.