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异烟肼-利福平诱导大鼠脂质变化。

Isoniazid-rifampicin induced lipid changes in rats.

作者信息

Pal R, Rana S V, Vaiphei K, Singh K

机构信息

Department of Gastroenterology, Postgraduate Institute of Medical Education and Research, Chandigarh, India.

出版信息

Clin Chim Acta. 2008 Mar;389(1-2):55-60. doi: 10.1016/j.cca.2007.11.028. Epub 2007 Dec 5.

Abstract

INTRODUCTION

Isoniazid (INH) and rifampicine (RIF) continues to be highly effective drugs in the chemoprophylaxis and treatment of tuberculosis. It is associated with hepatotoxicity in some individuals. Change in liver and serum lipids may be one of the reasons of hepatotoxicity. We examined isoniazid-rifampicine induced lipid changes in liver and serum of rats.

METHODS

In a rat model of INH-RIF induced hepatotoxicity we evaluated the effect of oral administration of INH-RIF (50 mg/kg body weight /day each) on hepatic marker enzymes, total lipids, cholesterol, triglycerides and phospholipids in serum and liver of experimental rats after 28 days. Enzymes, total lipids and lipid fractions were measured according to standard methods.

RESULTS

Treatment with INH-RIF increased the hepatic marker enzymes after 28 days and altered the lipid levels in serum and liver. Administration of INH-RIF resulted in significantly increased liver and serum cholesterol and total Lipids as compared to control group, while triglycerides were significantly elevated in liver only. In contrast, phospholipids were significantly decreased in liver and no effect in serum was observed.

CONCLUSION

Changes in lipids (both in serum and liver) are likely involved in the pathogenesis of INH-RIF induced hepatoxicity in rats.

摘要

引言

异烟肼(INH)和利福平(RIF)仍然是结核病化学预防和治疗中非常有效的药物。在一些个体中,它与肝毒性有关。肝脏和血清脂质的变化可能是肝毒性的原因之一。我们研究了异烟肼-利福平诱导的大鼠肝脏和血清脂质变化。

方法

在异烟肼-利福平诱导的肝毒性大鼠模型中,我们评估了口服异烟肼-利福平(各50mg/kg体重/天)对实验大鼠28天后血清和肝脏中肝脏标志物酶、总脂质、胆固醇、甘油三酯和磷脂的影响。根据标准方法测量酶、总脂质和脂质组分。

结果

28天后,异烟肼-利福平治疗使肝脏标志物酶升高,并改变了血清和肝脏中的脂质水平。与对照组相比,异烟肼-利福平给药导致肝脏和血清胆固醇及总脂质显著增加,而仅肝脏中的甘油三酯显著升高。相反,肝脏中的磷脂显著减少,血清中未观察到影响。

结论

脂质变化(血清和肝脏中)可能参与了异烟肼-利福平诱导的大鼠肝毒性的发病机制。

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