Peer-reviewed veterinary case report
Skin lymphoma tumors at vaccine sites in 17 cats studied
By Roccabianca, P et al.·Published in Veterinary pathology·2016·University of Milano, Italy·View original on PubMed →
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Original publication title: Cutaneous Lymphoma at Injection Sites: Pathological, Immunophenotypical, and Molecular Characterization in 17 Cats.
- Species:
- cat
Plain-English summary
A group of 17 cats, mostly male domestic short-haired and averaging 11 years old, developed skin tumors at the sites of vaccine injections. These tumors, known as cutaneous lymphomas, appeared anywhere from 15 days to nearly 9 years after the injections. Most of the cats showed no signs of internal disease at the time of diagnosis. The tumors were characterized by significant tissue damage and inflammation. Treatments varied, but understanding the type of lymphoma helped guide care.
People also search for: cat skin tumor after vaccine · feline lymphoma symptoms · cat injection site tumor treatment
Abstract
Feline primary cutaneous lymphomas (FPCLs) account for 0.2% to 3% of all lymphomas in cats and are more frequently dermal nonepitheliotropic small T-cell tumors. Emergence of FPCL seems unrelated to feline leukemia virus (FeLV) serological positivity or to skin inflammation. A total of 17 cutaneous lymphomas with a history of vaccine injection at the site of tumor development were selected from 47 FPCLs. Clinical presentation, histology, immunophenotype, FeLV p27 and gp70 expression, and clonality were assessed. A majority of male (12/17), domestic short-haired (13/17) cats with a mean age of 11.3 years was reported. Postinjection time of development ranged from 15 days to approximately 9 years in 5 cats. At diagnosis, 11 of 17 cats had no evidence of internal disease. Lymphomas developed in interscapular (8/17), thoracic (8/17), and flank (1/17) cutaneous regions; lacked epitheliotropism; and were characterized by necrosis (16/17), angiocentricity (13/17), angioinvasion (9/17), angiodestruction (8/17), and peripheral inflammation composed of lymphoid aggregates (14/17). FeLV gp70 and/or p27 proteins were expressed in 10 of 17 tumors. By means of World Health Organization classification, immunophenotype, and clonality, the lesions were categorized as large B-cell lymphoma (11/17), anaplastic large T-cell lymphoma (3/17), natural killer cell-like (1/17) lymphoma, or peripheral T-cell lymphoma (1/17). Lineage remained uncertain in 1 case. Cutaneous lymphomas at injection sites (CLIS) shared some clinical and pathological features with feline injection site sarcomas and with lymphomas developing in the setting of subacute to chronic inflammation reported in human beings. Persistent inflammation induced by the injection and by reactivation of FeLV expression may have contributed to emergence of CLIS.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/26933095/