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首页> 外文期刊>Journal of drug research. >Ultra Structural And Biochemical Studies On The Effects Of Natural And Synthetic Anti-Fibrotic Drugs On Liver Of Schistosoma Mansoni Infected Mice When Given With Anti-Schistosomal Treatment
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Ultra Structural And Biochemical Studies On The Effects Of Natural And Synthetic Anti-Fibrotic Drugs On Liver Of Schistosoma Mansoni Infected Mice When Given With Anti-Schistosomal Treatment

机译:天然和合成抗纤维化药物联合抗血吸虫治疗对曼氏血吸虫感染小鼠肝脏的超结构和生化研究

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Schistosoma mansoni is one of the most prevalent causes of liver fibrosis in Egypt. Liver fibrosis is the result of an imbalance between synthesis and degradation of extracellular matrix proteins of the liver. This progressive process is mainly characterized by activation of hepatic stellate cells (HSCs). Colchicine is a well known drug used for treating liver fibrosis, however higher doses cannot be used due to its toxicity. Silymarin is a natural acknowledged hepatoprotector used in humans to treat liver diseases. The aim of this work was to evaluate the antifibrotic effects of colchicine (when given alone or combined with Silymarin) on liver of schistosomal infected mice model, treated with antibilharzial drug (Mirazid). Ninety mice were divided into 6 groups (15/group), the first served as non-infected control and the second as infected control. The infected mice of the 3~(rd), 4~(th), 5~(th) and 6~(th) groups were given mirazid, mirazid and colchicine, mirazid and Silymarin and mirazid, colchicine and Silymarin respectively. Histological (Light and Electron microscopical analysis) and biochemical tools were used. The current work showed that best results were achieved in group of animals treated with mirazid and administered combined colchicine and Silymarin. Electron microscope examination showed HSCs returned to approximately resting phase. Hepatocytes revealed normal appearing picture with normally seen microvilli surface. This was confirmed by light microscopic examination. Biochemical analysis of some liver functions (Total proteins, albumin, GGT, ALP and LDH), was in parallel with the histological results. We concluded that activation of HSCs may play a key role in the progress of Schistosoma induced hepatic fibrosis, and the use of Silymarin colchicine combined with antibilharzial drug reduces this activation.
机译:曼氏血吸虫是埃及肝纤维化最普遍的原因之一。肝纤维化是肝脏细胞外基质蛋白合成与降解之间失衡的结果。这种进行性过程的主要特征是肝星状细胞(HSC)的激活。秋水仙碱是用于治疗肝纤维化的众所周知的药物,但是由于其毒性而不能使用更高剂量。水飞蓟素是人类公认的天然肝保护剂,可用于治疗肝脏疾病。这项工作的目的是评估秋水仙碱(当单独或与水飞蓟素联合使用时)对血吸虫病感染小鼠模型的肝脏的抗纤维化作用,该小鼠接受了抗胆管炎药物(Mirazid)治疗。将90只小鼠分为6组(每组15只),第一组用作未感染的对照,第二组用作感染的对照。对第3,第4,第5和第6组的感染小鼠分别给予米拉西德,米拉西德和秋水仙碱,米拉西德和水飞蓟素和米拉西德,秋水仙碱和水飞蓟素。使用组织学(光和电子显微镜分析)和生化工具。当前的工作表明,在用咪拉吉德治疗并联合秋水仙碱和水飞蓟素治疗的动物组中取得了最佳结果。电子显微镜检查显示HSCs恢复到近似静止状态。肝细胞显示正常出现的图像,并具有正常可见的微绒毛表面。通过光学显微镜检查证实了这一点。对某些肝功能(总蛋白,白蛋白,GGT,ALP和LDH)的生化分析与组织学结果平行。我们得出的结论是,HSC的激活可能在血吸虫诱导的肝纤维化进展中起关键作用,而水飞蓟素秋水仙碱与抗胆道管药物联合使用可降低这种激活。

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