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尿胆汁酸作为大鼠肝损伤非侵入性指标的效能

Efficacy of urine bile acid as a non-invasive indicator of liver damage in rats.

作者信息

Kawai Hiroshi, Kudo Naomi, Kawashima Yoichi, Mitsumoto Atsushi

机构信息

Faculty of Pharmaceutical Sciences, Josai International University, 1 Gumyo, Togane, Chiba 283-8555, Japan.

出版信息

J Toxicol Sci. 2009 Feb;34(1):27-38. doi: 10.2131/jts.34.27.

Abstract

Estimation of liver damage is important in the pathophysiological and toxicological study of liver disease. As a novel, non-invasive marker of liver damage, we studied the efficacy of urine bile acids (UBA) in a rat model of liver disease. Thioacetamide (TAA)-treated rats were used in this study. Single intraperitoneal administration of high-dose TAA induces severe damage to the liver, and thus is used as a model of acute hepatitis. Continuous administration of low-dose TAA yields mild damage to the liver, and induces cirrhosis and hepatic tumors. In this study, it was found that both acute and chronic administration of TAA was associated with a dose-dependent elevation of UBA. The elevation of UBA content correlated with the alteration of blood biochemical indicators, and UBA screening showed a remarkable ability to distinguish liver-damaged rats from healthy rats. In particular, UBA analysis was found to have high sensitivity, specificity, and positive predictive value for the screening of rats with abnormal serum alkaline phosphatase (ALP) activity due to chronic liver damage, which was confirmed to include cholestasis and subsequent cirrhosis by liver histological analysis. In conclusion, we demonstrated that measurement of UBA is a simple, non-invasive and effective method for the screening of cholestasis in TAA-treated rats. We suggest that UBA analysis may have potent applicability for monitoring the progress of liver damage in animal models of chronic liver disease, such as cirrhosis and hepatic encephalopathy.

摘要

在肝脏疾病的病理生理学和毒理学研究中,评估肝损伤至关重要。作为一种新型的肝损伤非侵入性标志物,我们研究了尿胆汁酸(UBA)在大鼠肝脏疾病模型中的效能。本研究使用硫代乙酰胺(TAA)处理的大鼠。单次腹腔注射高剂量TAA会导致肝脏严重损伤,因此用作急性肝炎模型。连续给予低剂量TAA会对肝脏造成轻度损伤,并诱发肝硬化和肝肿瘤。在本研究中,发现急性和慢性给予TAA均与UBA的剂量依赖性升高有关。UBA含量的升高与血液生化指标的变化相关,并且UBA筛查显示出区分肝损伤大鼠和健康大鼠的显著能力。特别是,发现UBA分析对于筛查因慢性肝损伤导致血清碱性磷酸酶(ALP)活性异常的大鼠具有高灵敏度、特异性和阳性预测值,通过肝脏组织学分析证实其中包括胆汁淤积及随后的肝硬化。总之,我们证明了测量UBA是一种用于筛查TAA处理大鼠胆汁淤积的简单、非侵入性且有效的方法。我们建议UBA分析可能在监测慢性肝病动物模型(如肝硬化和肝性脑病)中肝损伤的进展方面具有强大的适用性。

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