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Peer-reviewed veterinary case report

Immune response and outcomes in dogs with bone cancer

By Mason, Nicola J et al.·Published in Molecular therapy : the journal of the American Society of Gene Therapy·2025·Department of Pathobiology, United States·View original on PubMed

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Original publication title: Immunological responses and clinical outcomes in dogs with osteosarcoma receiving standard therapy and a Listeria vaccine expressing HER2.

Species:
dog
OsteosarcomaMovement & jointsDogs

Plain-English summary

A group of dogs with bone cancer (osteosarcoma) received a new vaccine alongside standard treatment to see if it could help them live longer or prevent the cancer from spreading. The vaccine was generally well tolerated, with only mild side effects. While the vaccine did not significantly extend the overall survival or time without disease compared to dogs receiving standard treatment alone, some dogs showed stronger immune responses after multiple doses. This suggests that further studies could explore giving the vaccine more frequently to help improve outcomes for dogs with this type of cancer.

People also search for: dog osteosarcoma treatment · vaccine for dog cancer · how to help dog with bone cancer

Abstract

A clinical trial in dogs with spontaneous osteosarcoma was performed to assess a recombinant Listeria expressing a chimeric human HER2 (ADXS31-164) as an adjunctive vaccine strategy to prevent metastatic disease and determine immunological correlates of clinical outcome. A total of 118 dogs with appendicular osteosarcoma were recruited into a 1-arm, multicenter, prospective trial of standard of care (SOC) therapy followed by ADXS31-164. ADXS31-164was well tolerated, with mostly transient, low-grade side effects. Significant differences in median disease-free interval (DFI) or median overall survival (OS) of immunized dogs compared to a historical cohort of dogs receiving SOC only were not observed. Elite survivors (DFI >490 days) showed transient increases in temperature and serum cytokines, including IL-6 and TNF-α, after the first immunization compared to short-term survivors (DFI 150-235 days). However, repeat immunizations in short-term survivors led to improved and comparable pyrexic and cytokine responses to elite survivors. PBMC transcriptomic analysis following vaccinations revealed robust cytotoxic activity in elite but not short-term survivors. Although ADXS31-164did not significantly extend DFI or OS, immune responses to ADXS31-164distinguished elite from short-term survivors. Improvement of immune responses over sequential ADXS31-164administrations supports a future trial design of recurrent immunizations to improve outcomes of otherwise short-term survivors.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/39955616/