玛咖多糖对D-半乳糖衰老模型小鼠生殖器官的保护作用

目的:探讨玛咖多糖(MP)对D-半乳糖(D-gal)引起的衰老模型小鼠生殖器官损伤的保护作用。方法:将50只无特定病原体(SPF)级雄性癌症研究所(ICR)小鼠按体质量采用简单随机化(Simple Randomization)法分为空白组,模型组,MP低剂量组、MP中剂量组、MP高剂量组,每组10只。除空白组给予生理盐水外,其余组连续8周每天颈背部注射D-gal 500 mg/kg造模。MP低剂量组、MP中剂量组和MP高剂量组从造模起分别按75 mg/kg、150 mg/kg和300 mg/kg剂量连续8周每日灌胃MP。用透射电镜观察小鼠附睾组织形态,测定睾丸组织中谷胱甘肽过氧化物酶(GSH-Px)、丙二醛和单胺氧化酶(MAO)活力,并用实时聚合酶链式反应(PCR)检测附睾超氧化物歧化酶2(SOD 2)、过氧化氢酶表达情况,蛋白质免疫印迹法检测沉默信息调节因子1/P53信号通路中沉默信息调节因子1和P53蛋白的表达情况。结果:48 d后,MP各剂量组小鼠体质量增长高于模型组小鼠,差异有统计学意义(P<0.05);MP中剂量组睾丸指数和附睾指数较模型组升高(P<0.05)。与模型组比较,高剂量组小鼠睾丸组织中GSH-Px活力升高,丙二醛含量、MAO活力均下降(P<0.05);与模型组比较,MP高剂量组小鼠睾丸组织SOD 2、CAT在基因水平的表达增强;与模型组比较,MP各剂量组睾丸组织中沉默信息调节因子1在蛋白水平的表达均升高,P53在蛋白水平的表达均下降(P<0.05或P<0.01)。结论:MP可通过提高GSH-Px活力及SOD 2、CAT抗氧化酶在基因水平的表达,降低丙二醛、MAO活力,对沉默信息调节因子1/P53蛋白信号通路的调控作用,从而保护小鼠生殖器官。

Modulation of synaptic damage by Bushen Tiansui Decoction via the PI3K signaling pathway in an Alzheimer’s disease model

Objective To explore the therapeutic effect and mechanism of Bushen Tiansui Decoction(补肾填髓方,BSTSD)and its active component icariin on Alzheimer’s disease(AD).Methods(i)Animal experiments.This study conducted experiments using specific pathogen-free(SPF)grade male C57BL/6J wild-type(WT)mice and APP/PS1 double transgenic mice.The animals were divided into three groups:WT group(WT mice,n=5,receiving distilled wa-ter daily),APP/PS1 group(APP/PS1 double transgenic mice,n=5,receiving distilled water daily),and BSTSD group[APP/PS1 double transgenic mice,n=5,treated with BSTSD suspen-sion at a dosage of 27 g/(kg·d)for 90 d].Cognitive function was assessed using the Morris wa-ter maze(MWM).Post-experiment,hippocampal tissues were collected for analysis of pyra-midal cell and synaptic morphology through hematoxylin-eosin(HE)staining and transmis-sion electron microscopy(TEM).(ii)Cell experiments.The HT-22 cells were divided into con-trol group(untreated),Aβ_(25-35) group(treated with 20μmol/L Aβ_(25-35) for 24 h),icariin group(pre-treated with 20μmol/L icariin for 60 min,followed by 20μmol/L Aβ_(25-35) for an additional 24 h),and icariin+LY294002 group[treated with 20μmol/L icariin and 20μmol/L LY294002(an inhibitor of the phosphoinostitide 3-kinases(PI3K)signaling pathway)for 60 min,then exposed to 20μmol/L Aβ_(25-35) for 24 h],and cell viability was measured.Western blot was used to detect the expression levels of synapse-associated proteins[synaptophysin(SYP)and post-synaptic density-95(PSD-95)]and PI3K signaling pathway associated proteins[phosphorylat-ed(p)-PI3K/PI3K,p-protein kinase B(Akt)/Akt,and p-mechanistic target of rapamycin(mTOR)/mTOR].Results(i)Animal experiments.Compared with APP/PS1 group,BSTSD group showed that escape latency was significantly shortened(P<0.01)and the frequency of crossing the origi-nal platform was significantly increased(P<0.01).Morphological observation showed that pyramidal cells in the hippocampal CA1 region were arranged more regularly,nuclear stain-ing was uniform,and vacuole-like changes were reduced after BSTSD treatment.TEM showed that the length of synaptic active zone in BSTSD treatment group was increased com-pared with APP/PS1 group(P<0.01),and the width of synaptic gap was decreased(P<0.01).(ii)Cell experiments.Icariin had no obvious toxicity to HT-22 cells when the concentration was not more than 20μmol/L(P>0.05),and alleviated the cell viability decline induced by Aβ_(25-35)(P<0.01).Western blot results showed that compared with Aβ_(25-35) group,the ratios of p-PI3K/PI3K,p-Akt/Akt and p-mTOR/mTOR in icariin group were significantly increased(P<0.01),while the protein expression levels of SYP and PSD-95 were increased(P<0.01).These effects were blocked by LY294002(P<0.01).Conclusion BSTSD and icariin enhance cognitive function and synaptic integrity in AD mod-els and provide potential therapeutic strategies through activation of the PI3K/Akt/mTOR pathway.