尿代谢组学用于评估异烟肼暴露后肝脏中微囊状脂质积累。

Susan J Sumner, Jason P Burgess, Rodney W Snyder, James A Popp, Timothy R Fennell
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引用次数: 0

摘要

本研究旨在开发一种无创的肝微泡性脂质积累(MVLA)标志物,这是一种目前在人类肝活检后诊断出的组织病理学效应。在化学品和药物的动物研究中检测到MVLA,并在一些接触化学品或药物的人类中发生。由于MVLA是一种可逆的组织病理学,使用无创方法对MVLA进行早期检测,可以帮助临床医生治疗服用已知会诱发这种损伤的药物的患者。选择异烟肼(INH)作为这项研究的模型化合物,因为MVLA发生在接受包括INH在内的联合治疗的结核病(TB)患者中。本研究使用雄性大鼠,每天以0、10或300 mg/kg/天的剂量给药INH,持续8天。第1天和第8天分别取尿、血和肝。给药8天的4/9大鼠尿液核磁共振代谢组学显示与右、左、中肝叶MVLA相关(100%)。肝脏提取物的代谢组学也揭示了与MVLA损伤相关的标志物。临床用于评估肝损伤的血清酶与MVLA的结果并不一致。代谢物变化与MVLA的存在一致,与肌醇、碳水化合物、甘油脂和乙醛酸代谢中断相关。本研究揭示了可以在临床前使用的标记物,为MVLA的机制提供了见解,并证明了在人类患者中验证无创MVLA标记物的必要性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Metabolomics of urine for the assessment of microvesicular lipid accumulation in the liver following isoniazid exposure.

Metabolomics of urine for the assessment of microvesicular lipid accumulation in the liver following isoniazid exposure.

Metabolomics of urine for the assessment of microvesicular lipid accumulation in the liver following isoniazid exposure.

Metabolomics of urine for the assessment of microvesicular lipid accumulation in the liver following isoniazid exposure.

This study was conducted to develop a noninvasive marker of hepatic microvesicular lipid accumulation (MVLA), a histopathological effect currently diagnosed in humans following liver biopsy. MVLA is detected in animal studies of chemicals and drugs and occurs in some humans exposed to chemicals or pharmaceuticals. Because MVLA is a reversible histopathology, early detection of MVLA using a noninvasive method, could aid clinicians in the treatment of patients taking drugs that are known to induce this injury. Isoniazid (INH) was selected as a model compound for this investigation, because MVLA occurs in tuberculosis (TB) patients treated with a combination therapy, which includes INH. This study used male rats dosed daily with INH at 0, 10, or 300 mg/kg/day for up to 8 days. Urine, blood, and liver were obtained following 1 and 8 days. NMR metabolomics of urine revealed markers that correlated (100%) with the findings of MVLA in the right, left, and median liver lobes in 4/9 rats administered the high dose of INH for 8 days. Metabolomics of liver extracts also revealed markers that correlated with the MVLA injury. Serum enzymes that are clinically used to assess liver injury were not consistently correlated to the findings of MVLA. Metabolite changes consistent with the presence of MVLA correlated with interruptions in inositol, carbohydrate, glycerolipid, and glyoxylate metabolism. This study reveals markers that could find pre-clinical use, provides insights into mechanisms involved in MVLA, and demonstrates the need for the validation of noninvasive MVLA markers in human patients.

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