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肝药酶诱导对动物和人类临床病理参数的影响。

Effects of hepatic drug-metabolizing enzyme induction on clinical pathology parameters in animals and man.

作者信息

Ennulat Daniela, Walker Dana, Clemo Frances, Magid-Slav Michal, Ledieu David, Graham Mark, Botts Suzanne, Boone Laura

机构信息

GlaxoSmithKline, King of Prussia, Pennsylvania 19406-0939, USA.

出版信息

Toxicol Pathol. 2010 Aug;38(5):810-28. doi: 10.1177/0192623310374332. Epub 2010 Jun 28.

Abstract

Hepatic drug-metabolizing enzyme (DME) induction is an adaptive response associated with changes in preclinical species; this response can include increases in liver weight, hepatocellular hyperplasia and hypertrophy, and upregulated tissue expression of DMEs. Effects of DME induction on clinical pathology markers of hepatobiliary injury and function in animals as well as humans are not well established. This component of a multipart review of the comparative pathology of xenobiotically mediated induction of hepatic metabolizing enzymes reviews pertinent data from retrospective and prospective preclinical and clinical studies. Particular attention is given to studies with confirmation of DME induction and concurrent evaluation of liver and/or serum hepatobiliary marker enzyme activities and histopathology. These results collectively indicate that in the rat, when histologic findings are limited to hepatocellular hypertrophy, DME induction is not expected to be associated with consistent or substantive changes in serum or plasma activity of hepatobiliary marker enzymes such as alanine aminotransferase, alkaline phosphatase, and gamma glutamyltransferase. In the dog and the monkey, published studies also do not demonstrate a consistent relationship across DME-inducing agents and changes in these clinical pathology parameters. However, increased liver alkaline phosphatase or gamma glutamyltransferase activity in dogs treated with phenobarbital or corticosteroids suggests that direct or indirect induction of select hepatobiliary injury markers can occur both in the absence of liver injury and independently of induction of DME activity. Although correlations between tissue and serum levels of these hepatobiliary markers are limited and inconsistent, increases in serum/plasma activities that are substantial or involve changes in other markers generally reflect hepatobiliary insult rather than DME induction. Extrahepatic effects, including disruption of the hypothalamic-pituitary-thyroid axis, can also occur as a direct outcome of hepatic DME induction in humans and animals. Importantly, hepatic DME induction and associated changes in preclinical species are not necessarily predictive of the occurrence, magnitude, or enzyme induction profile in humans.

摘要

肝药代谢酶(DME)诱导是一种与临床前物种变化相关的适应性反应;这种反应可包括肝脏重量增加、肝细胞增生和肥大,以及DMEs的组织表达上调。DME诱导对动物和人类肝胆损伤及功能的临床病理标志物的影响尚未完全明确。这部分关于异源物质介导的肝代谢酶诱导的比较病理学的多部分综述回顾了回顾性和前瞻性临床前及临床研究的相关数据。特别关注那些证实了DME诱导并同时评估肝脏和/或血清肝胆标志物酶活性及组织病理学的研究。这些结果共同表明,在大鼠中,当组织学发现仅限于肝细胞肥大时,预计DME诱导不会与肝胆标志物酶如丙氨酸转氨酶、碱性磷酸酶和γ-谷氨酰转移酶的血清或血浆活性的一致或实质性变化相关。在犬和猴中,已发表的研究也未表明DME诱导剂与这些临床病理参数变化之间存在一致的关系。然而,用苯巴比妥或皮质类固醇治疗的犬肝脏碱性磷酸酶或γ-谷氨酰转移酶活性增加表明,在无肝损伤且独立于DME活性诱导的情况下,可发生对特定肝胆损伤标志物的直接或间接诱导。尽管这些肝胆标志物的组织和血清水平之间的相关性有限且不一致,但血清/血浆活性的大幅增加或涉及其他标志物的变化通常反映肝胆损伤而非DME诱导。肝外效应,包括下丘脑-垂体-甲状腺轴的破坏,也可作为人类和动物肝DME诱导的直接结果而发生。重要的是,临床前物种中的肝DME诱导及相关变化不一定能预测人类中事件的发生、程度或酶诱导谱。

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