世界中医药
文章摘要
引用本文:杨晓伟1,张银环2,段飞鹏2,肖红斌2.基于Lable-free蛋白质组学技术研究大黄素致大鼠肝损伤作用机制[J].世界中医药,2019,(02):.  
基于Lable-free蛋白质组学技术研究大黄素致大鼠肝损伤作用机制
Study on Mechanism of Liver Injury in Rats Induced by Emodin Based on Lable-free Proteomics Technology
投稿时间:2018-01-18  
DOI:10.3969/j.issn.1673-7202.2019.02.014
中文关键词:  大黄素  蛋白质组学  肝损伤  组织蛋白酶  机制  半胱氨酸
English Keywords:Emodin  Protiomics  Liver injury  Cathepsin  Mechanism  Cysteine
基金项目:国家科学技术重大专项(2014ZX09304307);国家自然科学基金项目(81573839,81703948)
作者单位
杨晓伟1,张银环2,段飞鹏2,肖红斌2 1 中国中医科学院中药研究所北京100700 2 北京中医药大学中药分析与转化研究中心北京100029 
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中文摘要:
      目的:探索连续4周服用大黄素对大鼠肝组织蛋白表达的影响。方法:选取以大黄折算临床剂量100倍的大黄素灌胃SD大鼠4周(HG1,HG2,HG3,HG4)为模型,采用Lable-free蛋白质组学方法检测肝组织蛋白表达,并对所得结果进行分析。结果:通过筛选,HG1、HG2、HG3、HG4组中分别有158个、650个、219个、378个差异蛋白,这些差异蛋白经GO分析发现主要与细胞和代谢过程相关。其中,4组中共有差异蛋白25个,GO分类表明25个蛋白中有10个为与催化活性相关的蛋白。大黄素的存在使α-2-HS-糖蛋白(热稳定性糖蛋白)表达上调,该蛋白的浓度与肝病的严重程度正相关;并且组织蛋白酶家族蛋—富含半胱氨酸的蛋白酶表达下调。结论:长期服用大黄素会增加肝损伤的概率,其可能是由于含半胱氨酸蛋白酶的表达下调,使组织功能出现紊乱,导致肝损伤的出现,并且这一结果在低剂量组中也得到了印证。
English Summary:
      To investigate the influence of 4-week's emodin on protein expression of rat's liver tissue. Methods:SD rats were given emodin 100 times more than the clinical dose of Rhubarb for 4 weeks and were divided into four groups (HG1,HG2,HG3,HG4). Protein expression in liver tissue was detected by lable-free proteomic technology. Results:By screening, there were 158, 650, 219, and 378 differential proteins in HG1, HG2, HG3, and HG4 group respectively, which were found to be mainly associated with cellular and metabolic processes by GO analysis. Among them, there were 25 differential proteins in the four groups, and GO classification indicated that 10 of the 25 proteins were proteins related to catalytic activity. α-2-HS-glycoprotein (thermostable glycoprotein) expression was upregulated by the presence of emodin, and the concentration of this protein positively correlated with the severity of liver disease; and cathepsin family egg-cysteine-rich protease expression was downregulated. Conclusion:Long-term administration of emodin increases the probability of liver injury, which may be due to the down-regulation of the expression of cysteine-containing proteases, which leads to the disorder of tissue function and leads to the appearance of liver injury, and this result has also been confirmed in the low-dose group.
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