Expression of osteogenic proteins in kidneys of cats with nephrocalcinosis.

IF 2.6 2区农林科学

Journal of Veterinary Internal Medicine Pub Date : 2025-01-01 DOI:10.1111/jvim.17278

Nuttha Hengtrakul, Eva Furrow, Michael Borofsky, Ferenc Toth, Jody P Lulich

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Abstract

Background: Nephrocalcinosis is a common pathological finding in cats with chronic kidney disease and nephrolithiasis. Understanding its pathogenesis may identify future therapeutic targets.

Hypothesis: Nephrocalcinosis is associated with expression of an osteogenic phenotype.

Animals: Kidneys with medullary mineralization were obtained from 18 cats (10 with and 8 without nephroliths) undergoing necropsy.

Methods: Cross-sectional study. Microradiography and histopathology (modified von Kossa stain) were used to confirm parenchymal mineralization. Immunohistochemistry for 5 osteogenic markers was performed to determine their co-localization with nephrocalcinosis. The proportion of kidneys with stronger immunointensity in mineralized versus non-mineralized regions was analyzed using 1-tailed sign tests. The proportion of kidneys with co-localization of nephrocalcinosis and each marker was compared between kidneys with and without nephroliths using Fisher's exact tests.

Results: Nephrocalcinosis co-localized with osteopontin immunoreactivity in all 18 cats (100%) and with osteocalcin in 12 cats (67%). Both osteogenic markers had stronger immunointensity in mineralized regions compared with non-mineralized regions. Limited co-localization was observed with other markers: bone morphogenic protein-2 in 2 kidneys (both with nephroliths) and tissue non-specific alkaline phosphatase in 1 kidney (without nephroliths); runt-related transcription factor-2 was undetected. No statistically significant differences were found in the co-localization of nephrocalcinosis with osteogenic proteins between kidneys with and without nephroliths.

Conclusions and clinical importance: Expression of osteogenic proteins in areas of nephrocalcinosis indicates that nephrocalcinosis is associated with the development of an osteogenic phenotype. Targeting these processes could offer a novel approach to prevent nephrolithiasis at its origin.

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肾钙化症猫肾脏成骨蛋白的表达。

背景：肾钙质沉着症是猫慢性肾病和肾结石的常见病理表现。了解其发病机制可以确定未来的治疗靶点。假设：肾钙质沉着症与成骨表型的表达有关。动物：从尸检的18只猫（10只有肾结石，8只没有肾结石）身上获得肾髓质矿化。方法：横断面研究。显微x线摄影和组织病理学（改良von Kossa染色）证实实质矿化。对5种成骨标志物进行免疫组化，以确定它们与肾钙质沉着症的共定位。采用单尾标志试验分析矿化区与非矿化区免疫强度较强的肾脏比例。采用Fisher精确试验比较有肾结石和无肾结石肾脏中肾钙化共定位及各标志物的比例。结果：18只猫肾钙沉着症均伴有骨桥蛋白免疫反应（100%），12只猫伴有骨钙素免疫反应（67%）。两种成骨标志物在矿化区比非矿化区具有更强的免疫强度。与其他标志物有限的共定位：2个肾脏（均有肾结石）的骨形态发生蛋白-2和1个肾脏（无肾结石）的组织非特异性碱性磷酸酶；未检测到矮子相关转录因子-2。在有肾结石和没有肾结石的肾脏中，伴有成骨蛋白的肾钙化症共定位没有统计学上的显著差异。结论和临床意义：肾钙化症区成骨蛋白的表达表明肾钙化症与成骨表型的发展有关。针对这些过程可以提供一种新的方法来预防肾结石的起源。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Veterinary Internal Medicine Veterinary-General Veterinary

自引率

11.50%

发文量

243

期刊介绍： The mission of the Journal of Veterinary Internal Medicine is to advance veterinary medical knowledge and improve the lives of animals by publication of authoritative scientific articles of animal diseases.