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Noninvasive mapping of the redox status of dimethylnitrosamine-induced hepatic fibrosis using in vivo dynamic nuclear polarization-magnetic resonance imaging

机译:使用体内动态核极化-磁共振成像的无创映射二甲基亚硝胺诱导的肝纤维化的氧化还原状态。

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摘要

Hepatic fibrosis is a chronic disorder caused by viral infection and/or metabolic, genetic and cholestatic disorders. A noninvasive procedure that enables the detection of liver fibrosis based on redox status would be useful for disease identification and monitoring, and the development of treatments. However, an appropriate technique has not been reported. This study describes a novel method for assessing the redox status of the liver using in vivo dynamic nuclear polarization-magnetic resonance imaging (DNP-MRI) with the nitroxyl radical carbamoyl-PROXYL as a molecular imaging probe, which was tested in dimethylnitrosamine-treated mice as a model of liver fibrosis. Based on the pharmacokinetics of carbamoyl-PROXYL in control livers, reduction rate mapping was performed in fibrotic livers. Reduction rate maps demonstrated a clear difference between the redox status of control and fibrotic livers according to the expression of antioxidants. These findings indicate that in vivo DNP-MRI with a nitroxyl radical probe enables noninvasive detection of changes in liver redox status.
机译:肝纤维化是由病毒感染和/或代谢,遗传和胆汁淤积性疾病引起的慢性疾病。一种能够基于氧化还原状态检测肝纤维化的非侵入性程序,对于疾病的识别和监测以及治疗方法的开发将是有用的。但是,尚未报道适当的技术。这项研究描述了一种新的方法,该方法通过使用体内动态核极化磁共振成像(DNP-MRI)和亚硝酰基自由基氨基甲酰基-PROXYL作为分子成像探针来评估肝脏的氧化还原状态,该方法已在二甲基亚硝胺治疗的小鼠中进行了测试作为肝纤维化的模型。基于氨基甲酰-PROXYL在对照肝脏中的药代动力学,在纤维化肝脏中进行了降速映射。还原速率图表明,根据抗氧化剂的表达,对照组和纤维化肝脏的氧化还原状态之间存在明显差异。这些发现表明,具有硝基氧基自由基探针的体内DNP-MRI能够无创检测肝脏氧化还原状态的变化。

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