Peer-reviewed veterinary case report
c-kit gene types and prognosis in dog mammary tumors
By Chen, Yi-Chen et al.·Published in Veterinary and comparative oncology·2020·Graduate Institute of Veterinary Pathobiology·View original on PubMed →
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Original publication title: Expression frequency of c-kit isoforms and its prognostic potential in canine mammary tumours.
- Species:
- dog
Plain-English summary
A study looked at the levels of certain proteins (c-kit isoforms) in 196 samples from dogs with mammary tumors, both benign and malignant. It found that these proteins were present in higher amounts in tumors compared to normal tissue. Interestingly, dogs with high-grade malignant tumors had lower levels of one specific protein, which was linked to a shorter survival time. This suggests that measuring these protein levels could help predict how well a dog with malignant mammary tumors might do.
People also search for: dog mammary tumor prognosis · c-kit protein in dogs · canine breast cancer survival rates
Abstract
KIT is a tyrosine kinase receptor involved in carcinogenesis. Two alternatively spliced transcripts, differed from presence of four amino acids (GNSK) at exon 9 of c-kit, were identified in various human tumours and canine hemangiosarcoma (HSA). The biological function and clinical implications of these isoforms have not yet been elucidated in canine tumours. The current study aimed to validate the expression profile and ultimately to evaluate the correlation of c-kit isoform levels with clinicopathological factors of canine mammary tumours (CMTs). In total, the expression profiles of c-kit isoforms in 196 samples obtained from normal mammary glands (NMGs) of healthy controls and dogs with CMTs, benign and malignant CMTs, and HSAs were determined by polymerase chain reaction (PCR) and quantified via real-time PCR. Overall, the expression levels of the two isoforms were equivalent in NMGs, whereas the GNSK/GNSKratio sharply increased to 7.44- and 8.33-fold, indicating abundant GNSKisoforms in benign and malignant CMTs, respectively. However, a significant decrease in GNSKexpression was detected in dogs with high-grade malignant CMTs (mCMTs) and with metastatic CMTs compared with expression in those with a lower grade and non-metastatic CMTs. In addition, the median survival time was shorter in mCMT canines with a lower GNSK/GNSKratio than that in mCMT canines with a higher ratio (899 days vs 1534 days). In conclusion, two c-kit isoforms are ubiquitously expressed with great variability in HSAs and CMTs with both benign and malignant status. The GNSK/GNSKratio could serve as a prognostic indicator for dogs with mCMTs.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/31652393/