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Peer-reviewed veterinary case report

New photosensitizer drug tested for pet cancer light therapy

By Borgatti‐Jeffreys, A. et al.·Published in Veterinary and Comparative Oncology·2005·View original on Crossref

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Original publication title: A Candidate Second‐Generation Photosensitizer for Photodynamic Therapy in Veterinary Medicine

Species:
dog

Plain-English summary

A Golden Retriever with a large malignant tumor was treated with a new light-activated drug called ZnPcS4 as part of a clinical trial for photodynamic therapy (PDT). After the treatment, the tumor appeared dark and dead, indicating that the therapy was effective, and there were no harmful side effects noted in the dog. The owner reported that their pet did not experience any adverse reactions following the treatment. While the initial results are promising, more research is needed to fully understand how this treatment can be used safely in veterinary medicine.

People also search for: dog tumor treatment · photodynamic therapy for dogs · Golden Retriever cancer treatment

Abstract

Introduction: Photodynamic therapy (PDT) involves the light activation of a drug within a tumor causing selective tumor cell death. Unfortunately, some photosensitizing drugs have been associated with adverse reactions in veterinary patients. Zinc phthalocyanine tetrasulfonate (ZnPcS4) is a promising second‐generation photosensitizer for use in veterinary medicine, however, it cannot be applied clinically until safety and efficacy data are available.Methods: Increasing intraperitoneal doses of ZnPcS4 were given to Swiss Webster mice to assess acute toxicity. Based on mouse toxicity data, a phase I clinical trial of ZnPcS4‐based PDT in tumor‐bearing dogs was designed, using an accelerated titration scheme starting at 0.5% of the minimum toxic dose in mice. 24‐hours after ZnPcS4 administration tumors were irradiated with 675 nm light and dogs were evaluated by routine hematology and serum biochemistry at regular intervals after PDT.Results: Doses >125 mg/kg were associated with acute toxicity and mortality in Swiss Webster mice, suggesting the minimum toxic dose is 120–125 mg/kg. One dog, a Golden retriever with a massive malignant fibrous histiocytoma, has been entered into the phase I clinical trial. No deleterious effects were noted after ZnPcS4 administration. Within 48 hours of PDT, the tumor was dark and necrotic, with no grossly visible changes to the surrounding normal tissues. Histological examination of the PDT‐treated tumor confirmed widespread necrosis and thrombosis consistent with PDT‐mediated damage. The owner reported no adverse effects after treatment.Conclusions: Although preliminary data are encouraging, additional evaluation of ZnPcS4‐based PDT is required to determine its role in veterinary medicine.

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Original publication on Crossref: https://doi.org/10.1111/j.1476-5810.2005.064aa.x