Peer-reviewed veterinary case report
MicroRNA-21 and tumor markers in dog mammary tumors
By Ramadan, Eman S et al.·Published in Veterinary research communications·2022·Department of Internal Medicine and Infectious Diseases·View original on PubMed →
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Original publication title: MicroRNA-21 expression, serum tumor markers, and immunohistochemistry in canine mammary tumors.
- Species:
- dog
Plain-English summary
A group of 10 female dogs with mammary tumors had their blood tested for specific markers to help understand their condition. The study found that a marker called miR-21 was significantly higher in these dogs compared to healthy ones, suggesting it could be a useful indicator of mammary tumors. Additionally, another marker, CA 15-3, was elevated in all dogs with tumors. The findings indicate that measuring miR-21 might help veterinarians diagnose and monitor canine mammary tumors more effectively.
People also search for: dog mammary tumor symptoms · elevated miR-21 in dogs · canine cancer blood tests
Abstract
BACKGROUND: Canine mammary tumors (CMTs) are one of the most common malignancies in dogs and are associated with significant mortality. Serum tumor markers and non-coding microRNAs have gained widespread popularity in human oncology studies. The present study has two aims, first one is to investigate the miR-21 expression compared with changes in serum tumor markers (CEA and CA15-3) in CMT. The second aim is to detect the immunohistochemistry markers as vimentin, P63, and -SMA in CMT. METHODS: This study enrolled 17 female dogs: 10 with mammary tumors and seven controls without tumors. Blood samples were collected to measure miR-21, CEA, and CA 15-3, and histological samples were prepared for histological grading and immunohistochemistry. RESULTS: CA 15-3 was elevated in all animals, whereas CEA levels showed no change compared with controls. miR-21 was upregulated 12.84-fold in animals with CMT. The most frequently recorded CMT was the mixed type. Myoepithelial cells were identified by P63 immunoreactivity, but not SMA. High expression of miR-21 was observed with positive vimentin immunoreactivity, indicating the mesenchymal origin of the tumor cells. CONCLUSION: The present study showed that miR-21 was elevated to a greater extent than CA 15-3 (12.84-fold vs. threefold). Tumors that was positive for vimentin immunoreactivity was also associated with an elevation in the levels of miR-21, showing that miR-21 is released from mesenchymal cells. These findings support the hypothesis that miR-21 may be a more sensitive, noninvasive indicator for CMT.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/34787777/