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Peer-reviewed veterinary case report

Kidney tissue changes in cats with chronic kidney disease

By White, Joanna D et al.·Published in Journal of comparative pathology·2021·Sydney School of Veterinary Science, United Kingdom·View original on PubMed

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Original publication title: Renal Crest Proliferative Lesions in Cats with Chronic Kidney Disease.

Species:
cat

Plain-English summary

A study found that many cats with chronic kidney disease (CKD) showed abnormal growths in their kidney tissue. Out of 90 cats examined, 64% had some form of epithelial proliferation, which can range from mild changes to more serious conditions like cancer. Some cats had hyperplasia, which is an increase in the number of cells, while others had more severe changes, including invasive carcinomas. This suggests that if your cat has CKD, it's important to monitor for potential kidney tissue changes, as they can lead to serious health issues.

People also search for: cat chronic kidney disease symptoms · cat kidney cancer signs · treatment for cat kidney disease

Abstract

In a histopathological study of the renal crest (RC) of kidneys of cats with chronic kidney disease (CKD), 58/90 (64%) had epithelial proliferation. Of these, 33 cats had hyperplasia of the collecting duct (CD) epithelium (CDH) alone, eight had hyperplasia of the urothelium covering the RC (RCUH), of which one had concurrent abaxial renal pelvic urothelial hyperplasia (UH), and eight had both CDH and RCUH. CDH or RCUH were present in five cats with marked dysplasia of the CD epithelium (CDD) and four cats with invasive carcinomas, which also had epithelial dysplasia. All nine cats with marked dysplasia or neoplasia of the RC also had substantially altered RC contours due to focal haemorrhage, papillary necrosis or fibrosis. Three of the carcinomas had a strong desmoplastic response. In control cats, both urothelial (RC and renal pelvis) and tubular (CD and distal tubular) cells were immunopositive for cytokeratin (CK; AE1/AE3), tubular epithelial cells were positive for vimentin (Vim) and aquaporin 2 (Aq2), while urothelial cells were positive for p63. PAX8 immunolabelling was difficult to validate. CD and UH labelling was similar to control tissue. While urothelial dysplasia had the same immunolabelling pattern as UH and control tissue, CDD was generally immunonegative for Aq2. As immunolabelling of the four carcinomas did not distinguish between tubular and urothelial origin, with three positive for both Vim and p63, all were broadly designated as RC carcinomas. Overall, proliferative epithelial lesions are common in cats with CKD and form a continuum from simple hyperplasia to neoplasia of the urothelium or CD of the RC.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/34503654/