Puerarin protects rat brain against ischemia/reperfusion injury by suppressing autophagy via the AMPK-mT OR-ULK1 signaling pathway

Puerarin suppresses autophagy to alleviate cerebral ischemia/reperfusion injury, and accumulating evidence indicates that the AMPKm TOR signaling pathway regulates the activation of the autophagy pathway through the coordinated phosphorylation of ULK1. In this study, we investigated the mechanisms underlying the neuroprotective effect of puerarin and its role in modulating autophagy via the AMPK-m TOR-ULK1 signaling pathway in the rat middle cerebral artery occlusion model of cerebral ischemia/reperfusion injury. Rats were intraperitoneally injected with puerarin, 50 or 100 mg/kg, daily for 7 days. Then, 30 minutes after the final administration, rats were subjected to transient middle cerebral artery occlusion for 90 minutes. Then, after 24 hours of reperfusion, the Longa score and infarct volume were evaluated in each group. Autophagosome formation was observed by transmission electron microscopy. LC3, Beclin-1 p62, AMPK, m TOR and ULK1 protein expression levels were examined by immunofluorescence and western blot assay. Puerarin substantially reduced the Longa score and infarct volume, and it lessened autophagosome formation in the hippocampal CA1 area following cerebral ischemia/reperfusion injury in a dose-dependent manner. Pretreatment with puerarin（50 or 100 mg/kg） reduced Beclin-1 expression and the LC3-II/LC3-I ratio, as well as p-AMPK and p S317-ULK1 levels. In comparison, it increased p62 expression. Furthermore, puerarin at 100 mg/kg dramatically increased the levels of p-m TOR and p S757-ULK1 in the hippocampus on the ischemic side. Our findings suggest that puerarin alleviates autophagy by activating the APMK-m TOR-ULK1 signaling pathway. Thus, puerarin might have therapeutic potential for treating cerebral ischemia/reperfusion injury.

真武汤对大部分肾切除所致尿毒症心肌病小鼠心脏的保护作用

目的探讨真武汤对小鼠尿毒症心肌病心脏保护作用及其机制。方法大部分肾切除术制作尿毒症心肌病模型。C57BL/6小鼠随机分3组:假手术组、模型组和真武汤组。真武汤组小鼠术后予真武汤灌胃,假手术组和模型组小鼠术后予等量蒸馏水灌胃。心脏彩超、心脏组织HE染色及血生化分别观察尿毒症心肌病小鼠心脏功能、结构及肾功能变化,Western blotting检测心脏组织p-AMPK及p-mTOR的表达情况。结果模型组小鼠较假手术组体质量明显下降(P<0.05),心脏质量及心脏指数明显增加(P<0.05),心脏舒张期及收缩期左室后壁厚度增大(P<0.05),HE染色示心肌细胞肥大,血尿素氮、肌酐显著升高(P<0.05)。真武汤组小鼠与模型组相比心脏质量及心脏指数减小(P<0.05),心脏舒张期及收缩期左室后壁厚度减小(P<0.05),病理变化减轻。模型组小鼠与假手术组相比p-AMPK表达明显降低,p-mTOR表达明显升高(P<0.05);真武汤组小鼠与模型组相比pAMPK表达明显升高,p-mTOR表达明显降低(P<0.05)。结论真武汤抑制尿毒症心肌病小鼠心肌肥厚,此效应可能是通过AMPK-mTOR信号通路实现。

大黄酚介导AMPK依赖性信号通路抑制结肠癌SW480细胞的增殖、侵袭和裸鼠体内肿瘤形成

目的:以体外培养SW480细胞和体内荷瘤裸鼠为研究对象,探讨大黄酚(Chr)对结肠癌SW480细胞增殖、侵袭和裸鼠体内肿瘤形成的影响。方法:分别在结肠癌细胞SW480中加入25、50和100μmol/L大黄酚,Brdu染色法检测细胞增殖情况,Western blot检测增殖相关蛋白Ki67和PCNA表达水平;划痕实验和Transwell实验检测细胞迁移及侵袭能力;Western blot检测VEGF、E-cadherin和N-cadherin等上皮间充质转化相关蛋白表达,免疫荧光法检测波形蛋白表达情况;Western blot检测信号通路AMPK、mTOR和cyclin D1表达;建立移植瘤裸鼠模型,分别腹腔注射12.5、25和50 mg/kg大黄酚,检测荷瘤小鼠存活率、肿瘤重量,采用免疫组织化学法检测肿瘤组织中Ki67和PCNA表达水平,Western blot检测信号通路AMPK、mTOR和cyclin D1活化情况。结果:体外实验表明,大黄酚能剂量依赖性地抑制人结肠癌SW480细胞增殖和Ki67、PCNA蛋白表达(P<0.05或P<0.01),降低细胞划痕闭合率和侵袭细胞数量(P<0.05或P<0.01),调节E-cadherin、VEGF、N-cadherin、Vimentin、AMPK、mTOR和cyclin D1在SW480细胞中的表达水平(P<0.05或P<0.01);体内实验表明,与对照组(0.45±0.09)g相比,大黄酚各剂量组肿瘤组织重量分别为(0.32±0.06)g、(0.24±0.07)g和(0.15±0.04)g,差异具有统计学意义(P<0.05或P<0.01),且大黄酚剂量依赖性地抑制Ki67和PCNA表达(P<0.05或P<0.01),调控AMPK、p-mTOR和cyclin D1在肿瘤组织的表达(P<0.05或P<0.01)。结论:大黄酚通过AMPK信号通路抑制结肠癌SW480细胞的增殖、侵袭及荷瘤小鼠肿瘤形成。

竹节参皂苷IVa减轻异丙肾上腺素诱导的小鼠心肌纤维化作用机制研究

目的:探讨竹节参皂苷(IVa)减轻异丙肾上腺素(ISO)诱导的小鼠心肌纤维化作用机制。方法:白变种实验室老鼠(Balb/C)小鼠40只并随机分为4组:正常对照组(n=10)、ISO模型组(n=10)、IVa低剂量组(n=10)、IVa高剂量组(n=10)。采用皮下注射ISO构建小鼠心肌纤维化模型,IVa剂量组在建模同时给予IVa治疗,正常组给予等量生理盐水。采用马松(Masson)三色标准和HE染色方法分析评估心脏组织形态学和胶原沉积。采用小麦胚芽凝集素(WGA)染色法测定心肌细胞面积。蛋白免疫印迹试验检测细胞自噬相关标志物(LC3-Ⅱ、Beclin1和p62)和腺苷单磷酸活化蛋白激酶(AMPK)/哺乳动物雷帕霉素靶蛋白(m TOR)/自噬激活激酶1(ULK1)信号通路相关标志物。采用酶联免疫吸附法(ELISA)检测血清中血管紧张素II(Ang II)和I型前胶原羧基末端肽(PICP)的含量。结果:高剂量IVa(15mg/kg)治疗后,HW/BW和LVW/BW较ISO模型组升高,而血清中Ang II和PICP含量降低。IVa以剂量依赖的方式减轻心肌细胞在心脏组织中的损伤。皮下注射ISO后,心肌间质内胶原沉积明显,IVa治疗后胶原沉积明显减少。IVa可有效降低ISO诱导的小鼠心肌细胞面积大小。IVa能有效抑制ISO诱导的LC3-Ⅱ和Beclin1蛋白降低,减少p62蛋白增多。AMPK直接磷酸化ULK1(Ser555),通过抑制m TOR磷酸化间接抑制ULK1(Ser757)磷酸化,均参与了ISO诱导的心肌纤维化小鼠自噬活性的降低;此外,IVa低剂量组和IVa高剂量组均显著增加了AMPK磷酸化,并抑制了m TOR磷酸化,降低了ULK1(Ser757)磷酸化。结论:IVa通过AMPK/m TOR/ULK1途径激活自噬,减轻了ISO诱导的心肌纤维化。表明IVa是一种潜在的抗心肌纤维化候选药物,是治疗心脏病的潜在药物靶点。