经皮穴位电刺激复合药物全麻行控制性降压至不同水平对肝血流的影响

目的探讨经皮穴位电刺激(transcutaneous electrical acupoint stimulation,TEAS)复合药物全麻行控制性降压至不同水平的肝血流变化,从而明确针药复合麻醉的肝保护效应机制。方法 42只雄性比格犬随机分为7组:单纯全麻组、50%对照组、50%实验组、40%对照组、40%实验组、30%对照组和30%实验组,每组6只,后6组动物均以异氟醚联合硝普钠行控制性降压,将动脉血压降至50%、40%、30%基础平均动脉血压(mean arterial pressure,MAP)水平并维持60min,单纯全麻组不行控制性降压。实验组采用TEAS干预处理,刺激强度(4±1)mA,频率2/100Hz,穴位选用犬双侧"合谷(LI4)"、"足三里(ST36)"、"三阴交(SP6)"、"曲池(LI11)",电刺激在动物生理状态稳定后开始至维持目标MAP60min后停止。采用激光多普勒组织血流仪监测不同水平相应时间点肝组织表面血流的变化。结果在控制性降压开始至目标低血压维持结束,50%对照组肝血流在各时间点均显著低于同期单纯全麻组和基础水平(P<0.05),而50%实验组仅在维持30～60min阶段显著降低,且在维持阶段早期(10～30min),50%实验组肝血流显著高于同期对照组(P<0.05),而40%、30%各水平实验组肝血流无明显升高。在血压回升阶段(20～30min),40%实验组肝血流已先后恢复到同期单纯全麻组水平和基础水平,而对照组尚未恢复;在此阶段,50%、30%实验组和对照组肝血流有相似的变化趋势。结论在行控制性降压至50%水平时,TEAS的肝保护效应在降压、维持阶段早期体现明显。在行控制性降压至40%时,TEAS的肝保护效应在血压回升阶段体现明显。

Research on the protection effect of pioglitazone for non-alcoholic fatty liver disease (NAFLD)in rats

Objective： The prevalence of non-alcoholic fatty liver disease （NAFLD） has markedly increased. Insulin resistance has been implicated in the pathogenesis of NAFLD. This study was aimed at observing the relationship between insulin resistance and NAFLD, and evaluating the role of pioglitazone （PGZ） acting as insulin-sensitizing agents in the prevention and treatment of rat fatty liver induced by high fat feeding. Methods： The rats were separated randomly into 6 groups： model group Ⅰ were fed high fat diet for 8 weeks, PGZ prevention group were given PGZ 4 mg/（kg.d） simultaneously, while control group Ⅰ were fed normal food for 8 weeks; model group Ⅱ were fed high fat diet for 16 weeks, PGZ treatment group were given PGZ 4 mg/（kg.d） orally simultaneous with high fat diet for 8 weeks after high fat feeding for 8 weeks, control group Ⅱ were fed normal food for 16 weeks. The rats were sacrificed after 8 weeks and 16 weeks respectively. Liver weight, body weight, serum activities of alanine aminotransferase （ALT）, aspartate aminotransferase （AST）, alkaline phosphatase （ALP）, tumor necrosis factor alpha （TNF-α）, fasting blood glucose （FBG）, fasting plasma insulin （FINS）, HOMA （homeostasis model assessment） insulin resistance index （HOMA-IR）, and the liver histology of rats of all groups were assayed. Results： After 8 weeks, the liver in model group Ⅰ showed typical steatosis, accompanied with mild to moderate lobular inflammatory cell infiltration, liver indexes and serum levels of ALT, AST, ALP, TNF-α were significantly increased （P〈0.05） compared with control group Ⅰ. Whereas, the degree of hepatic injury was attenuated in PGZ prevention group, liver indexes and serum levels of ALT, ALP were significantly decreased （P〈0.05） compared with model group Ⅰ. After 16 weeks, notable steatosis, and lobular inflammation were observed in model group Ⅱ rat liver, while the degree of hepatic injury was attenuated in the PGZ treatment group. Liver index, serum levels ofALT, AST, ALP, FINS and HOMA-IR were significantly increased （P〈0.05） in model group Ⅱ compared with control group Ⅱ. Whereas, in PGZ treatment group, serum levels of AST and FINS showed decreasing tendency, liver indexes, serum levels of ALT, ALP, TNF-α and HOMA-IR were significantly decreased compared with model group Ⅱ. Conclusion： Insulin resistance plays a role in the pathogenesis of NAFLD in rats. Pioglitazone can attenuate insulin resistance and biochemical and histological injury in high fat-induced fatty liver in rats.