Peer-reviewed veterinary case report
Cat with itchy bleeding skin tumors resistant to toceranib treatment
By Hiroyuki Tani et al.·Published in Veterinary Medicine and Science·2024·Laboratory of Veterinary Radiology Department of Veterinary Medicine College of Bioresource Sciences Nihon University Fujisawa Kanagawa Japan, GB·View original on DOAJ →
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Original publication title: A case report of feline mast cell tumour with intertumoral heterogeneity: Identification of secondary mutations c.998G>C and c.2383G>C in KIT after resistance to toceranib
- Species:
- cat
Plain-English summary
A 12-year-old male domestic cat with multiple lumps under the skin was brought in after experiencing itching and raw, bleeding skin from scratching for two weeks. The cat was initially treated with two different chemotherapy drugs, vinblastine and nimustine, but neither worked. Eventually, a medication called toceranib was given, which initially helped the cat's tumors shrink completely. However, two months later, the tumors stopped responding to toceranib due to new mutations in the tumor cells. This case highlights the complexity of treating mast cell tumors in cats and suggests that more research is needed to find effective treatments.
People also search for: cat skin lumps treatment · feline mast cell tumor symptoms · toceranib for cats · cat itching and bleeding skin · mast cell tumor chemotherapy for cats
Abstract
Abstract A 12‐year‐old male domestic cat with multiple subcutaneous mast cell tumours (MCTs) presented with a 2‐week history of pruritus and raw/bleeding skin from self‐trauma at Kagoshima University Veterinary Teaching Hospital. Polymerase chain reaction (PCR) and histopathological analyses revealed intertumoral heterogeneity among tumour locations based on the mutation status of KIT. In addition, the expression pattern of KIT was characterized. After failed treatment with vinblastine (2.0–2.2 mg/m2, intravenous administration, two doses in total) or nimustine (25 mg/m2, intravenous administration, two doses in total), toceranib (2.2–2.6 mg/kg, orally administered, every other day) was administered to treat recurrent MCTs harbouring the KIT exon eight internal tandem duplication mutation, achieving a complete response. However, toceranib resistance developed 2 months after treatment initiation. Subsequent PCR analysis was conducted to identify the mutational status of KIT in each MCT and to detect the presence of secondary mutations associated with the acquisition of toceranib resistance. Secondary KIT mutations (c.998G>C and c.2383G>C), which were not initially detected in tumour cells at diagnosis, were identified after the development of resistance to toceranib. This indicates that the tumour cells in feline MCTs in the same case have diverse characteristics. Our findings encourage further investigation into the development of therapeutic strategies for feline MCTs, particularly focusing on the heterogeneous nature of KIT/KIT and overcoming acquired resistance to toceranib.
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Search related cases →Original publication on DOAJ: https://doi.org/10.1002/vms3.70003