澳大利亚犬的铜肝病

IF 1.3 4区 农林科学 Q2 VETERINARY SCIENCES Australian Veterinary Journal Pub Date : 2024-04-29 DOI:10.1111/avj.13338
J Mutton, S Yeomans, J White
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引用次数: 0

摘要

引言根据世界小动物兽医协会(WSAVA)指南评估澳大利亚犬只的肝病。材料和方法对小动物专科医院的医疗记录进行审查,以确定在 2008 年 11 月至 2021 年 11 月期间患有肝病并进行了肝活检的犬只。肝脏组织病理学报告由一名获得兽医病理学家资格认证的兽医进行审查,并根据 WSAVA 指南进行分类。对组织病理学报告和临床记录进行审查,以确定最重要的组织学过程,从而进行统计分析。铜相关性肝病的定义是:(i) 组织学证据显示中央叶区(3 区)有铜积聚,并伴有肝细胞坏死、含铜巨噬细胞的炎症和慢性肝炎;(ii) 组织化学铜染色显示中央叶区有肝细胞铜积聚;(iii) 肝脏铜测量值大于 600 μg/g 干重。患有原发性炎症实质疾病的犬包括铜相关性肝病、特发性慢性肝炎、非特异性反应性肝炎、慢性细菌性肝炎和免疫介导的慢性肝炎。对所有犬只进行了描述性统计。比较了铜相关性肝病和其他原因引起的慢性原发性炎症性实质肝病的狗的年龄、体重和临床病理数据(Kruskal-Wallis 检验)。计算并比较铜相关性肝病患犬与其他慢性原发性炎症性实质肝病患犬的存活时间(Kaplan-Meier 曲线和对数秩检验)。对犬的品种进行了评估,以确定最常患铜相关性肝病的犬种,并找出以前未曾描述过这种疾病的犬种。结果共纳入 67 只犬(43 只雌犬,24 只雄犬),中位年龄为 7.8 岁(四分位 [Q] Q1-Q3 4.5-9.6 岁)。其中 13 只狗患有铜相关性肝病,8 只狗患有特发性慢性肝炎,8 只狗患有非特异性反应性肝炎,7 只狗患有门静脉高压症相关疾病,5 只狗患有慢性细菌性肝炎,4 只狗患有免疫介导的慢性肝炎。与其他原因引起的慢性原发性炎症性实质肝病的狗相比,铜相关性肝病的狗往往更年轻(6.73 岁对 8.01 岁,P = 0.057)、更重(19.8 千克对 9.6 千克,P = 0.052)。ALT (P = 0.30)、ALP (P = 0.18)和总胆红素(P = 0.13)在两组之间的比较没有统计学差异。结论铜相关性肝病在患有慢性肝病的澳大利亚犬中很常见,与其他原因引起的原发性炎症性实质肝病相比,铜相关性肝病多发于年龄较小、体重较大的犬。临床病理学对于区分铜相关性肝病和其他原因引起的慢性原发性炎症性实质肝病并无帮助。如果铜相关性肝病得到治疗,预后会很好。这是首次报告澳大利亚查理士王小猎犬患铜相关性肝病。
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Copper hepatopathies in Australian dogs

Introduction

To evaluate hepatopathies in Australian dogs according to the World Small Animal Veterinary Association (WSAVA) guidelines. Specifically, to describe the prevalence and survival of dogs with copper-associated hepatopathy.

Materials and methods

Medical records from the Small Animal Specialist Hospital were reviewed to identify dogs with liver disease and liver biopsy between November 2008 and November 2021. Liver histopathology reports were reviewed with a board-certified veterinary pathologist and classified according to the WSAVA guidelines. Histopathology reports and clinical records were reviewed to ascertain the most important histological process for statistical analysis. Copper-associated hepatopathy was defined as (i) histological evidence of copper accumulation in centrilobular areas (Zone 3) associated with hepatocyte necrosis, inflammation with copper-laden macrophages and chronic hepatitis (ii) histochemical copper staining showing hepatocyte copper accumulation in the centrilobular areas and iii) hepatic copper measurement with concentrations greater than 600 μg/g dry weight of liver. Dogs with primary inflammatory parenchymal disease included dogs with copper-associated hepatopathy, idiopathic chronic hepatitis, non-specific reactive hepatitis, chronic bacterial hepatitis and immune-mediated chronic hepatitis. Descriptive statistics were performed for all dogs. Age, weight and clinicopathologic data were compared between dogs with copper-associated hepatopathy and dogs with other causes of chronic primary inflammatory parenchymal liver disease (Kruskal–Wallis test). Survival times were calculated and compared (Kaplan–Meier curves and log rank test) between dogs with copper-associated hepatopathy and dogs with other chronic primary inflammatory parenchymal liver diseases. Breed was evaluated to determine the breed most commonly affected with copper-associated hepatopathy and identify any breed in which this disease has not previously been described.

Results

Sixty-seven (43 female, 24 male) dogs with a median age of 7.8 years (quartile [Q] Q1-Q3 4.5–9.6 years) were included. Thirteen dogs had copper-associated hepatopathy, eight dogs had idiopathic chronic hepatitis, eight dogs had non-specific reactive hepatitis, seven dogs had disorders associated with portal hypertension, five dogs had chronic bacterial hepatitis and four dogs had immune-mediated chronic hepatitis. Compared with dogs with other causes of chronic primary inflammatory parenchymal liver disease, dogs with copper-associated hepatopathy tended to be younger (6.73 vs. 8.01 years, P = 0.057) and heavier (19.8 vs. 9.6 kg, P = 0.052) than dogs with other causes of primary chronic inflammatory parenchymal diseases. There was no statistically significant difference when ALT (P = 0.30), ALP (P = 0.18) and total bilirubin (P = 0.13) were compared between the two groups.

The median survival time for all dogs after liver biopsy was 2010 days (CI 1321 days – not reached). There was no significant difference in survival between dogs with copper-associated hepatopathy and dogs with other causes of chronic primary inflammatory parenchymal liver disease (P = 0.5).

Conclusions

Copper-associated hepatopathy was common among Australian dogs with chronic hepatopathies, occurring in younger and heavier dogs than other causes of primary inflammatory parenchymal liver disease. Clinical pathology is not useful for differentiating between copper-associated hepatopathy and other causes of chronic primary inflammatory parenchymal liver disease. When copper-associated hepatopathy is treated, the prognosis can be good. This is the first report of copper-associated hepatopathy in Australian Cavalier King Charles Spaniels.

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来源期刊
Australian Veterinary Journal
Australian Veterinary Journal 农林科学-兽医学
CiteScore
2.40
自引率
0.00%
发文量
85
审稿时长
18-36 weeks
期刊介绍: Over the past 80 years, the Australian Veterinary Journal (AVJ) has been providing the veterinary profession with leading edge clinical and scientific research, case reports, reviews. news and timely coverage of industry issues. AJV is Australia''s premier veterinary science text and is distributed monthly to over 5,500 Australian Veterinary Association members and subscribers.
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