枝莲保肝茶的制备及临床治疗慢性乙型病毒性肝炎疗效观察

目的:介绍枝莲保肝茶的处方组成、制备方法、质量标准和临床应用。方法:90例患者随机分组,治疗组70例,口服枝莲保肝茶;对照组20例,口服益肝灵分散片。3个月为1个疗程,1个疗程后检测ALT、TBIL、HbeAg转阴HBV-DNA、各种症状均有明显改善,来评定疗效。结果:两组比较有显著差异(P<0.05);治疗组各项指标改善情况明显优于对照组(P<0.05)。结论:枝莲保肝茶制备方法设计科学,在治疗慢性乙型病毒性肝炎临床疗效确切。

藤茶保肝片的制备工艺研究

目的:探讨藤茶保肝片的制备工艺。方法:采用正交试验优化提取工艺,通过单因素试验考察填充剂和黏合剂的种类。结果:提取工艺中藤茶最佳提取条件:提取时间0.5 h,料液比1∶8,提取次数3次;茯苓、绿豆、高良姜最佳提取条件:提取时间1.0 h,料液比1∶6,提取次数3次;成型工艺选择淀粉作为填充剂,4%淀粉浆为黏合剂。结论:该制备工艺简单,制得的藤茶保肝片外观光洁美观,质量符合要求。

保肝降脂泡袋茶治疗脂肪肝药理疗效分析

目的:研究分析我院自主配制的保肝降脂泡袋茶治疗脂肪肝药理机制观察临床疗效。方法:通过对脂肪肝致病因素的干预,引用相关文献对治疗前后的血脂、肝脏B超、肝功能检查结果、临床症状进行统计。结果:保肝降脂泡袋茶治疗脂肪肝有效率达到84.3%,血脂、肝脏B超、肝功能检查结果、临床症状均有明显改善。结论:保肝降脂泡袋茶治疗脂肪肝药理机制明确,临床疗效显著,值得临床推广。

保肝降脂泡袋茶治疗非酒精性脂肪肝80例临床研究

目的:观察保肝降脂泡袋茶治疗非酒精性脂肪肝的疗效。方法:将160例符合诊断标准的患者随机分为两组,各80例。治疗组应用保肝降脂泡袋茶,对照组给予东宝肝泰片治疗。12周为1个疗程,对比治疗前后的临床症状。结果:治疗组临床痊愈、显效、有效、无效分别为38例、36例、3例、3例,总有效率为92.5%;对照组临床痊愈、显效、有效、无效分别为24例、22例、15例、19例,总有效率有76.25%。x2检验结果显示,治疗后两组有显著性差异(P<0.05)。结论:保肝降脂泡袋茶治疗非酒精性脂肪肝疗效确切,未见不良反应。

保肝明目茶的制备工艺研究

目的:拟开发一款保肝明目茶,优选其最佳制备工艺。方法:以总多糖含量为评估指标,选用Design-Expert软件设计实验,优化水提工艺;以吸湿率、成形率、溶化性和含水量作为指标,选用正交设计,优选最佳制粒工艺。结果:最终确定的水提工艺:处方中的四味药材加12倍量水,提取温度80℃、提取时间2 h。最佳制粒工艺:取相对密度为1.25~1.30的浸膏,加入3倍浸膏量的赋形剂(玉米糊精∶可溶性淀粉=1∶4),再加入矫味剂甜菊糖0.25%,柠檬酸0.4%,混合制软材,制粒,干燥,整粒,即得。结论:优选的制备工艺稳定可行,为后期产品研发奠定了基础。

Protective effect of tea polyphenols against paracetamol-induced hepatotoxicity in mice is significanly correlated with cytochrome P450 suppression

AIM： To investigate the hepatoprotective activity of tea polyphenols （TP） and its relation with cytochrome P450 （CYP450） expression in mice. METHODS： Hepatic CYP450 and CYPbs levels were measured by UV-spectrophotometry in mice 2 d after intraperitoneal TP （25, 50 and 100 mg/kg per day）. Then the mice were intragastricly pre-treated with TP （100, 200 and 400 mg/kg per day） for six days before paracetamol （1000 mg/kg） was given. Their acute mortality was compared with that of control mice. The mice were pre-treated with TP （100, 200, and 400 mg/kg per day） for five days before paracetamol （500 mg/kg） was given. Hepatic CYP2E1 and CYPIA2 protein and mRNA expression levels were evaluated by Western blotting, immunohistochemical staining and transcriptase-polymerase chain reaction. RESULTS： The hepatic CYP450 and CYPb5 levels in mice of TP-treated groups （100, 200 and 400 mg/kg per day） were decreased in a dose-dependent manner compared with those in the negative control mice.TP significantly attenuated the paracetamol-induced hepatic injury and dramatically reduced the mortality of paracetamol-treated mice. Furthermore, TP reduced CYP2E1 and CYPIA2 expression at both protein and mRNA levels in a dose-dependent manner. CONCLUSION： TP possess potential hepatoprotective properties and can suppress CYP450 expression.