四氯化碳剂量(CCl4)对老鼠(Rattus norvegicus L)的有效性。作为动物肝脏纤维化的模型

F. Fahrudin, S. Ningsih, Hajar Indra Wardhana, Dinda Rama Haribowo, F. Hamida
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引用次数: 0

摘要

肝损伤可引起急性和慢性纤维化。肝纤维化动物模型的发展为获得新的治疗实体提供了宝贵的信息。本研究的目的是获得CCl4诱导实现肝纤维化动物模型的最佳条件。用椰子油稀释CCl4,连续口服6周。25只雄性大鼠分为5个治疗组,P1为正常组(不含CCl4)。P2 (CCl4 40%), 1 ml/kg bw,每周3次。P3 (CCl4 40%)、0.5 ml/kg bw每周3次、P4 (CCl4 10%) 1 ml/kg bw每周3次、P5 (CCl4 10%) 1 ml/kg bw每周2次。分析肝酶活性、宏观和微观肝损伤、大鼠死亡率。本研究结果显示,各治疗组肝酶含量均高于对照组(P<0.05)。肝组织病理学分析显示相同的结果。然而,如果观察大鼠死亡的百分比,P5与所有治疗组相比表现出最低的水平。由此可见,CCl4(10%)能较好地建立肝纤维化动物模型。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
EFEKTIVITAS DOSIS KARBON TETRAKLORIDA (CCl4) TERHADAP TIKUS (Rattus norvegicus L.) SEBAGAI HEWAN MODEL FIBROSIS HATI
Liver damage can produce fibrosis condition both acute and chronic. Development of liver fibrosis in animal models is valuable information in order to gain new entities for treatment. The aim of this study is to get an optimal condition of CCl4 induction for achieving animal models of liver fibrosis. CCl4 diluted in coconut oil was administrated orally for 6 consecutive weeks. Total 25 male rats were divided into 5 treatment groups, namely, P1 was a normal group (without CCl4). P2 (CCl4 40%), 1 ml/kg bw 3 times a week. P3 (CCl4 40%), 0.5 ml/kg bw 3 times a week, P4 (CCl4 10%) 1 ml/kg bw 3 times a week, and P5 (CCl4 10%) 1 ml/kg bw twice a week. The analyzed parameters were the activity of liver enzymes, macro and microscopic liver damage, and the percentage of rat deaths. The results of this study indicated an increase in liver enzymes in all treatments which was higher than P1 (P<0.05). Analysis of liver histopathology exhibeted the same result. However, if viewed the percentage of rat deaths, P5 demonstrated the lowest compared to all treatment groups. It could be concluded  that the administration of CCl4 (10%) was able to create an animal model of liver fibrosis optimally.  
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