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Assessment of amiodarone-induced phospholipidosis in chimeric mice with a humanized liver

机译:用人源化肝脏评估嵌合小鼠中胺碘酮诱导的磷脂

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It is important to consider susceptibility to drug-induced toxicity between animals and humans. Chimeric mice with a humanized liver are expected to predict hepatotoxicity in humans. Drug induced phospholipidosis (DIPL), in which phospholipids accumulate, is a known entity. In this study, we examined whether chimeric mice can reveal species differences in DIPL. Changes in various phosphatidylcholine (PhC) molecules were investigated in the liver of chimeric mice after administering amiodarone, which induces phospholipidosis. Liquid chromatography-tandem mass spectrometry revealed that levels of PhCs tended to increase in the liver after administration of amiodarone. The liver of chimeric mice consists of human hepatocytes and residual mouse hepatocytes. We used imaging mass spectrometry (IMS) to evaluate the increase of PhCs in human and mouse hepatocytes after administration of amiodarone. IMS visualizes localization of endogenous and exogenous molecules in tissues. The IMS analysis suggested that the localized levels of several PhCs tended to be higher in the human hepatocytes than those in mouse hepatocytes, and PhC levels changed in response to amiodarone. Chimeric mice with a humanized liver will be useful to evaluate species differences in DIPL between mice and humans.
机译:重要的是要考虑对动物和人类之间的药物诱导的毒性易感性。预期具有人源化肝脏的嵌合小鼠预测人类的肝毒性。药物诱导的磷脂(DIPL),其中磷脂积聚,是已知实体。在这项研究中,我们检查了嵌合小鼠是否可以揭示商品中的物种差异。在施用胺碘酮后,在嵌合小鼠的肝脏中研究了各种磷脂酰胆碱(PHC)分子的变化,该氨基酮诱导磷脂。液相色谱 - 串联质谱表明,在施用胺碘酮后,PHC的水平趋于增加肝脏。嵌合小鼠的肝脏由人肝细胞和残留的小鼠肝细胞组成。我们使用成像质谱(IMS)来评估胺碘酮后的人和小鼠肝细胞中PHC的增加。 IMS可视化组织中内源和外源分子的定位。 IMS分析表明,在人肝细胞的几个PHC的局部水平倾向于比小鼠肝细胞的肝细胞更高,并且对胺碘酮的响应而改变PHC水平。具有人源化肝脏的嵌合小鼠将有助于评估小鼠和人类之间的商品的物种差异。

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