Wu Yao-Ming, Joseph Brigid, Berishvili Ekaterine, Kumaran Vinay, Gupta Sanjeev
Marion Bessin Liver Research Center, Diabetes Center, Cancer Research Center, Department of Medicine, Albert Einstein College of Medicine, Bronx, New York 10461, USA.
Hepatology. 2008 Jan;47(1):279-87. doi: 10.1002/hep.21937.
The potential for organ damage after using drugs or chemicals is a critical issue in medicine. To delineate mechanisms of drug-induced hepatic injury, we used transplanted cells as reporters in dipeptidyl peptidase IV-deficient mice. These mice were given phenytoin and rifampicin for 3 days, after which monocrotaline was given followed 1 day later by intrasplenic transplantation of healthy C57BL/6 mouse hepatocytes. We examined endothelial and hepatic damage by serologic or tissue studies and assessed changes in transplanted cell engraftment and liver repopulation by histochemical staining for dipeptidyl peptidase IV. Monocrotaline caused denudation of the hepatic sinusoidal endothelium and increased serum hyaluronic acid levels, along with superior transplanted cell engraftment. Together, phenytoin, rifampicin, and monocrotaline caused further endothelial damage, reflected by greater improvement in cell engraftment. Phenytoin, rifampicin, and monocrotaline produced injury in hepatocytes that was not apparent after conventional tissue studies. This led to transplanted cell proliferation and extensive liver repopulation over several weeks, which was more efficient in males compared with females, including greater induction by phenytoin and rifampicin of cytochrome P450 3A4 isoform that converts monocrotaline to toxic intermediates. Through this and other possible mechanisms, monocrotaline-induced injury in the endothelial compartment was retargeted to simultaneously involve hepatocytes over the long term. Moreover, after this hepatic injury, native liver cells were more susceptible to additional pro-oxidant injury through thyroid hormone, which accelerated the kinetics of liver repopulation.
Transplanted reporter cells will be useful for obtaining insights into homeostatic mechanisms involving liver cell compartments, whereas targeted injury in hepatic endothelial and parenchymal cells with suitable drugs will also help advance liver cell therapy.
使用药物或化学物质后器官损伤的可能性是医学中的一个关键问题。为了阐明药物性肝损伤的机制,我们在二肽基肽酶IV缺陷小鼠中使用移植细胞作为报告物。给这些小鼠服用苯妥英钠和利福平3天,之后给予野百合碱,1天后进行健康C57BL/6小鼠肝细胞的脾内移植。我们通过血清学或组织学研究检查内皮和肝脏损伤,并通过二肽基肽酶IV的组织化学染色评估移植细胞植入和肝脏再填充的变化。野百合碱导致肝窦内皮剥脱和血清透明质酸水平升高,同时移植细胞植入情况良好。苯妥英钠、利福平与野百合碱共同导致进一步的内皮损伤,表现为细胞植入有更大改善。苯妥英钠、利福平和野百合碱对肝细胞造成损伤,这在传统组织学研究后并不明显。这导致移植细胞增殖和数周内广泛的肝脏再填充,雄性比雌性更有效,包括苯妥英钠和利福平对细胞色素P450 3A4亚型的诱导作用更强,该亚型将野百合碱转化为有毒中间体。通过这种及其他可能机制,野百合碱诱导的内皮区损伤在长期内被重新定位,同时累及肝细胞。此外,在这种肝损伤后,天然肝细胞通过甲状腺激素更容易受到额外的促氧化损伤,这加速了肝脏再填充的动力学。
移植的报告细胞将有助于深入了解涉及肝细胞区室的稳态机制,而用合适药物对肝内皮细胞和实质细胞进行靶向损伤也将有助于推进肝细胞治疗。
Zotero 插件