Peer-reviewed veterinary case report
Dog with mast cell tumor and c-kit mutation improved with imatinib
By Yamada, Osamu et al.·Published in Veterinary immunology and immunopathology·2011·Department of Veterinary Clinical Pathology, Japan·View original on PubMed →
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Original publication title: Imatinib elicited a favorable response in a dog with a mast cell tumor carrying a c-kit c.1523A>T mutation via suppression of constitutive KIT activation.
- Species:
- dog
Plain-English summary
A dog with a mast cell tumor on its right front paw was treated with imatinib, a targeted cancer medication. The tumor shrank significantly within just two weeks, and the dog's blood showed no signs of cancer cells. After five weeks, the swollen lymph node that had been affected by the cancer returned to normal size. This case suggests that imatinib can be effective for dogs with mast cell tumors, especially those with specific genetic mutations.
People also search for: dog mast cell tumor treatment · imatinib for dogs · mast cell tumor symptoms in dogs
Abstract
Target therapy using the tyrosine kinase inhibitor imatinib is one of the new therapeutic approaches for canine mast cell tumors (MCTs). In the present report, we demonstrate a clinical response to imatinib in a dog with MCT carrying a c-kit c.1523A>T mutation. Moreover, the effect of this mutation on the phosphorylation status of KIT and the inhibitory potency of imatinib on the phosphorylation of the mutant KIT were examined in vitro. A dog with a MCT tumor mass on the right forelimb sole with lymph node metastasis and mastocytemia was treated with imatinib. The MCT mass markedly shrank and mastocytemia became undetectable with 2 weeks of treatment. The lymph node enlarged by metastasis became normal in size with 5 weeks of treatment. From the sequencing analysis of c-kit in tumor cells, a substitution mutation c.1523A>T that alters the amino acid composition (p.Asn508Ile) within the extracellular domain of KIT was identified. The mutant KIT expressed on 293 cells showed ligand-independent phosphorylation and imatinib suppressed this phosphorylation in a dose-dependent manner. From these findings, imatinib was considered to elicit a clinical response in a canine case of MCT via inhibition of the constitutively activated KIT caused by a c-kit c.1523A>T mutation.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/21561667/