Peer-reviewed veterinary case report
c-kit mutation testing in primary and metastatic dog mast cell tumors
By Marconato, L et al.·Published in Journal of veterinary internal medicine·2014·Centro Oncologico Veterinario, Italy·View original on PubMed →
PetCaseFinder translated the abstract of this peer-reviewed paper into plain English so pet owners can read it. We do not publish original research — every detail traces back to the citation above. How we work →
Original publication title: Concordance of c-kit mutational status in matched primary and metastatic cutaneous canine mast cell tumors at baseline.
- Species:
- dog
Plain-English summary
A group of 21 dogs with metastatic mast cell tumors (MCT) had both their primary and metastatic tumors tested for c-kit mutations before starting treatment. The results showed that the mutation status was the same in both the primary and metastatic tumors, meaning that testing either tumor can help guide treatment decisions. Additionally, three new mutations were found, but these did not seem to relate to the dogs' clinical features. This suggests that targeted therapies could be effective for treating metastatic MCT based on the mutation status.
People also search for: dog mast cell tumor treatment · c-kit mutation in dogs · metastatic cancer in dogs
Abstract
BACKGROUND: Mutation analysis of proto-oncogene c-kit (c-kit) is advisable before starting treatment with tyrosine kinase inhibitors in dogs with mast cell tumor (MCT), including those with metastatic disease. Testing is usually performed on primary tumors, assuming that c-kit mutation status does not change in metastasis. HYPOTHESIS/OBJECTIVES: To give an insight into the mutational processes and to make a recommendation on the use of c-kit mutational analysis in the clinical setting. ANIMALS: Twenty-one client-owned dogs with metastatic MCT. METHODS: Dogs undergoing resection or biopsy for both primary and matched metastatic MCT were prospectively enrolled. Total RNA or DNA was extracted from primary MCT and corresponding metastases. Exons 8, 9, and 11 were amplified by PCR and sequenced. Genetic features between primary MCT and metastases were compared. Their correlation with clinicopathologic features was investigated. RESULTS: Concordance (mutated or wild-type) of mutational status, evaluable in 21 primary and matched metastatic (20 nodal and 1 splenic) MCTs, was 100%. Three new c-kit mutations were identified. No significant correlation was detected between c-kit mutation and clinicopathologic features. CONCLUSIONS AND CLINICAL IMPORTANCE: Proto-oncogene c-kit mutational status is conserved between any primary and its matched secondary tumor, suggesting that both can be used for c-kit mutational testing. Targeted therapies might be also used to treat metastatic disease.
Find similar cases for your pet
PetCaseFinder finds other peer-reviewed reports of pets with the same symptoms, plus a plain-English summary of what was tried across them.
Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/24372836/