[No authors listed]
BACKGROUND:KIT is a tyrosine kinase growth factor receptor. High expression of KIT has been found in several tumors including canine hemangiosarcoma (HSA). This study investigated the correlation of KIT expression and c-kit sequence mutations in canine HSAs and benign hemangiomas (HAs). RESULTS:Immunohistochemistry (IHC) staining confirmed KIT expression in 94.4Â % (34/36) of HSAs that was significantly higher than 0Â % in HAs (0/16). Sequencing the entire c-kit coding region of HSAs and normal canine cerebellums (NCCs) revealed GNSK-deletion in exon 9. As for exon 9 genotyping by TA-cloning strategy, GNSK-deletion c-kit accounted for 48.6Â % (68/140) colonies amplified from12 KIT-positive HSAs, a significantly higher frequency than 14.1Â % (9/64) of colonies amplified from six NCCs. CONCLUSIONS:Due to the distinct expression pattern revealed by IHC, KIT might be used to distinguish benign or malignant vascular endothelial tumors. Moreover, the high incidence of GNSK-deletion c-kit in canine HSAs implicates KIT isoforms as possibly participating in the tumorigenesis of canine HSAs.
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