Peer-reviewed veterinary case report
RAS, FLT3, and C-KIT gene mutations found in dog leukemia cases
By Usher, Suzanne G et al.·Published in Experimental hematology·2009·Small Animal Teaching Hospital, United Kingdom·View original on PubMed →
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Original publication title: RAS, FLT3, and C-KIT mutations in immunophenotyped canine leukemias.
- Species:
- dog
Plain-English summary
A group of dogs suspected of having leukemia were tested for specific genetic mutations. Out of 74 dogs, 57 were confirmed to have leukemia, with the majority having acute forms of the disease. Researchers found that a significant number of these dogs had mutations in genes similar to those seen in human leukemia, including N-RAS and FLT3. This suggests that these genetic changes are common in dogs with acute leukemia, which could help veterinarians better understand and treat the condition.
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Abstract
OBJECTIVE: To determine the frequency of FLT3, C-KIT, and RAS mutations in canine leukemia patients. MATERIALS AND METHODS: Ethylenediamine tetra-acetic acid blood samples were recruited from dogs with suspected leukemia, categorized by quantitative and cytological evaluation and immunophenotyping. Flow cytometry was carried out using antibodies against CD3; CD3e; CD4; CD5; CD8; CD11a, b, c, and d; CD14; CD21; CD34; CD45 and 45RA; CD79a; CD90 (THY-1); major histocompatibility complex II; myeloperoxidase; MAC387; and neutrophil-specific antibody. Genomic DNA was extracted from whole blood and analyzed for mutations in N, H, and K-RAS, FLT3, and C-KIT genes by polymerase chain reaction and sequencing. RESULTS: Fifty-seven (77.0%) of 74 samples submitted from dogs with suspected leukemia had cytologically and immunophenotypically confirmed leukemia. There were 36 (63.2%) acute leukemias, 16 (28.1%) chronic, 3 (5.3%) prolymphocytic, 1 natural killer cell, and 1 chronic leukemia undergoing blast transformation. N-RAS mis-sense mutations were identified in 14 (25%) dogs with acute myeloid (AML) or lymphoid (ALL) leukemia, and also in one dog in the leukemic phase of lymphoma. Mutations in K-RAS were found in two dogs with AML. There were no H-RAS mutations. FLT3 internal tandem duplications were identified in three dogs with ALL, and a mis-sense mutation was found in one dog with ALL. C-KIT mutations were identified in three dogs with AML. Sixty-one percent of dogs with acute leukemia harbored mutations in N/K-RAS, FLT3, or C-KIT. CONCLUSION: RAS, FLT3, and C-KIT mutations, analogous to those found in human leukemia, occur commonly in acute canine leukemia.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/18977066/