Peer-reviewed veterinary case report
Feline leukemia virus protein found in injection-site sarcoma
By Roccabianca, Paola et al.·Published in Veterinary pathology·2026·Università, Italy·View original on PubMed →
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Original publication title: Clonality assessment and feline leukemia virus protein expression in injection-site sarcoma-associated lymphocytic infiltrates.
- Species:
- cat
Plain-English summary
A 12-year-old male domestic shorthair cat developed a tumor at the site of a previous injection, known as feline injection-site sarcoma (FISS). Researchers examined 34 cases like this to understand the role of the feline leukemia virus (FeLV) in these tumors. They found that FeLV proteins were present in some of the tumor cells, suggesting that the virus might play a role in the development of these cancers. In one case, the cat had both FISS and cutaneous lymphoma, but it did not show FeLV expression. The findings indicate a potential link between FeLV and these types of tumors in cats.
People also search for: cat injection site tumor · feline leukemia virus and cancer · cat lymphoma symptoms · feline injection-site sarcoma treatment
Abstract
Injections have been linked to feline sarcomas (feline injection-site sarcoma; FISS) and cutaneous lymphomas (cutaneous lymphoma at injection site; CLIS). Both tumors often exhibit lymphoplasmacytic inflammation ascribed to injected immunogenic material. CLIS is hypothesized to emerge from transformation and clonal expansion of lymphoid cells following persistent immune stimulation with feline leukemia virus (FeLV) reactivation and transformation. To further study whether the lymphocytic infiltrates associated with FISS can represent a suitable niche for the development of CLIS, 34 cases of FISS were examined. Lymphoid cell phenotypes were assessed using CD3 and CD79 immunohistochemistry. For cases with prominent inflammation, FeLV p27 and gp70 immunohistochemistry and PCR for antigen receptor rearrangements were performed. Male domestic shorthair cats predominated. The mean age was 12.2 years (range: 5-17 years). FISS developed in thoracic (8/34, 24%), flank (7/34, 21%), and interscapular (5/34, 15%) regions. Similar proportions of B and T lymphocytes were found in 11/34 (32%) cases; T-cells predominated in 12/34 (35%) cases, and B-cells predominated in 11/34 (32%). At least one FeLV antigen was expressed in lymphoid infiltrates in 10/18 cases (55%), and in neoplastic fibroblasts in 8/18 cases (44%), while both FeLV proteins were expressed in neoplastic cells in 3/18 cases (17%). One cat had clonal T-cell receptor-gamma and was diagnosed with concurrent FISS and CLIS. This case lacked FeLV expression. FeLV amplification from formalin-fixed paraffin-embedded material was unsuccessful. The expression of FeLV p27 and/or gp70 in neoplastic spindle cells and lymphoid infiltrates raises the possibility of FeLV involvement in the tumorigenesis of FISS and CLISs.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/40914880/