腹腔神经丛阻滞对2型糖尿病Goto-Kakizaki大鼠胰岛的影响

目的观察腹腔神经丛阻滞(NCPB)对2型糖尿病Goto-Kakizaki(GK)大鼠胰腺的影响。方法 25只2型糖尿病(T2DM)构模成功的雄性GK大鼠,随机抽取5只取胰腺组织(N0),以观测基础状况;再随机将20只GK大鼠分为对照组和实验组,每组10只。实验组给予0.5%利多卡因行NCPB,1 ml/(次·d),对照组以0.9%生理盐水替换。对照组和实验组分别于14次(N14)和28次(N28)NCPB后,各取5只GK大鼠,取胰腺组织。采用免疫组化和Western blot法检测各组胰腺组织中TNF-α、IL-1β水平和Bax、Bcl-2的蛋白表达。结果 HE染色和胰岛素免疫组化分析均可见对照组和实验组GK大鼠胰腺在N14、N28时病变持续加重,胰岛数及细胞数目减少,并可见被增生纤维组织分割包围的胰岛明显萎缩,但两组相比,实验组胰岛萎缩程度明显轻于对照组;在N14、N28时,对照组胰岛的TNF-α和IL-1β水平均有所升高,而实验组却明显下降,并显著低于对照组;实验组GK大鼠胰腺Bax蛋白表达水平在N14、N28时显著低于对照组(P<0.01),Bcl-2蛋白表达显著高于对照组(P<0.01),Bax/Bcl-2比值显著低于对照组(P<0.01)。结论延缓T2DM模型GK大鼠胰岛的病理改变,可能是NCPB减轻糖耐量受损程度的机制之一。

2型糖尿病Goto-Kakizaki大鼠低三酰甘油血症及其作用途径

目的:观察2型糖尿病Goto-Kakizaki(GK)大鼠的三酰甘油代谢情况及其作用途径。方法:实验于2001-03/12在日本国立健康与营养研究所动物实验中心完成。选择8周龄GK大鼠30只及同龄对照Wistar大鼠21只,在11和15周龄测定GK大鼠和对照Wistar大鼠的血三酰甘油水平,在15周龄测定两类大鼠肝脏三酰甘油分泌速率、三酰甘油清除速率及脂蛋白脂酶活性。血浆三酰甘油测定应用酶法;血浆脂蛋白脂酶活性应用酶联免疫法法试剂盒测定;计算三酰甘油清除速率首先使用同位素标记的甘油测定血浆池体积,再将三酰甘油分泌速率除以血浆池体积。结果:GK大鼠30只及Wistar大鼠21只全部进入结果分析,无脱失。①两类大鼠血三酰甘油水平比较:在11和15周龄时,GK大鼠的空腹血浆三酰甘油水平明显低于同龄对照Wistar大鼠[(4.09±0.78,6.85±1.81;3.14±1.46,6.22±2.38)mmol/L(t=7.121,4.909,P<0.01)]。②两类大鼠肝脏三酰甘油分泌速率、三酰甘油清除速率、脂蛋白脂酶活性比较:在15周龄时,与对照Wistar大鼠相比,GK大鼠的肝脏三酰甘油分泌速率增高1.34倍,三酰甘油分解速率增高2.65倍,但肝素释放后的血浆脂蛋白脂酶活性与对照Wistar大鼠相比差异无显著性意义(P>0.05)。结论:GK糖尿病大鼠存在低三酰甘油血症,其可能作用途径是外周组织清除三酰甘油的能力高于肝脏产生和分泌三酰甘油的能力,造成血液中三酰甘油降低,从而出现低三酰甘油血症。

EGCG对Goto-kakizaki大鼠骨骼肌组织GLUT4表达的影响

目的 研究表没食子儿茶素没食子酸酯（EGCG）对自发性Ⅱ型糖尿病GK大鼠的作用及对骨骼肌组织葡萄糖转运蛋白4（GLUT4）表达的影响.方法 自发性2型糖尿病大鼠GK大鼠40只,同系健康对照Wistar大鼠10只,大鼠随机分为：正常对照组、Ⅱ型糖尿病组、Ⅱ型糖尿病低剂量EGCG（50 mg/kg）治疗组、中剂量（100 mg/kg）EGCG、高剂量EGCG（300 mg/kg）治疗组,6周后测血糖、血脂和骨骼肌GLUT4的水平.结果 EGCG可明显改善GK大鼠的OGTT及血脂,增加大鼠模型骨骼肌胞膜上GLUT4蛋白表达.结论 EGCG可降低TIIDM大鼠血糖水平,其机制与提高糖尿病大鼠骨骼肌中GLUT4表达有关.

Effect of berberine on hyperglycaemia and gut microbiota composition in type 2 diabetic Goto-Kakizaki rats

BACKGROUND A recent investigation showed that the prevalence of type 2 diabetes mellitus(T2DM)is 12.8%among individuals of Han ethnicity.Gut microbiota has been reported to play a central role in T2DM.Goto-Kakizaki(GK)rats show differences in gut microbiota compared to non-diabetic rats.Previous studies have indicated that berberine could be successfully used to manage T2DM.We sought to understand its hypoglycaemic effect and role in the regulation of the gut microbiota.AIM To determine whether berberine can regulate glucose metabolism in GK rats via the gut microbiota.METHODS GK rats were acclimatized for 1 wk.The GK rats were randomly divided into three groups and administered saline(Mo),metformin(Me),or berberine(Be).The observation time was 8 wk,and weight,fasting blood glucose(FBG),insulin,and glucagon-like peptide-1(GLP-1)were measured.Pancreatic tissue was observed for pathological changes.Additionally,we sequenced the 16S rRNA V3-V4 region of the gut microbiota and analysed the structure.RESULTS Compared with the Mo group,the Me and Be groups displayed significant differences in FBG(P<0.01)and GLP-1(P<0.05).A significant decrease in weight and homeostatic model assessment-insulin resistance was noted in the Be group compared with those in the Me group(P<0.01).The pancreatic islets of the Me-and Be-treated rats showed improvement in number,shape,and necrosis compared with those of Mo-treated rats.A total of 580 operational taxonomic units were obtained in the three groups.Compared to the Mo group,the Me and Be groups showed a shift in the structure of the gut microbiota.Correlation analysis indicated that FBG was strongly positively correlated with Clostridia_UCG-014(P<0.01)and negatively correlated with Allobaculum(P<0.01).Body weight showed a positive correlation with Desulfovibrionaceae(P<0.01)and a negative correlation with Akkermansia(P<0.01).Importantly,our results demonstrated that Me and Be could significantly decrease Bacteroidetes(P<0.01)and the Bacteroidetes/Firmicutes ratio(P<0.01).Furthermore,Muribaculaceae(P<0.01;P<0.05)was significantly decreased in the Me and Be groups,and Allobaculum(P<0.01)was significantly increased.CONCLUSION Berberine has a substantial effect in improving metabolic parameters and modulating the gut microbiota composition in T2DM rats.

Goto-Kakizaki大鼠十二指肠空肠旷置术模型的建立

目的探讨以Goto-Kakizaki(GK)大鼠建立保留全胃的十二指肠空肠旷置术(DJB)模型的可行性及操作要点。方法将16只GK大鼠随机分为实验组(n=8)和对照组(n=8)。在规范的术前、术中及术后操作下,对实验组和对照组大鼠分别行DJB术和假手术,比较2组大鼠术前,术后1、2、3及4周空腹血糖和体质量的变化情况,评价手术造模是否成功,并观察2组大鼠的存活情况。结果术后4周2组大鼠均全部存活。与术前比较,实验组术后1周空腹血糖即下降(P<0.05),术后2、3及4周血糖趋于稳定;对照组术后各时相空腹血糖水平无明显变化(P>0.05)。术后各时相实验组的空腹血糖水平均低于对照组(P<0.05),提示成功建立了模型。实验组术后4周体质量的增加值低于对照组(P<0.05)。结论 DJB是一种可行的、安全有效的降糖术式。规范实验操作程序可以降低术中风险,建立稳定的GK大鼠DJB模型。

不同年龄非肥胖2型糖尿病Goto-Kakizaki大鼠离体主动脉血管收缩与舒张功能

目的观察比较非肥胖2型糖尿病Goto-Kakizaki(GK)大鼠不同年龄时的血糖及血管收缩与舒张功能,探讨其功能变化的可能机制。方法实验采用6与40周龄雄性GK大鼠,每组6只,同龄Wistar大鼠作对照。记录体质量、血糖以及清醒状态下的尾动脉血压及心率后,麻醉开胸剪取胸主动脉,检测离体血管环的收缩功能及内皮依赖性与非内皮依赖性舒张功能,并留取血清测定胰岛素水平。结果①与Wistar大鼠比较,GK大鼠的血糖在6周龄[(8.1±0.4)比(5.8±0.3)mmol/L,P<0.01]、40周龄[(17.3±0.8)比(5.6±0.4)mmol/L,P<0.01]均明显升高,血压及胰岛素水平未见明显变化,40周龄GK大鼠心率较Wistar大鼠明显升高。②两组不同年龄GK大鼠血管对60mmol/L氯化钾及1×10-6～1×10-5mol/L苯肾上腺素的最大收缩反应均减弱,但去内皮后40周龄组GK血管对低剂量1×10-8mol/L苯肾上腺素的收缩反应增强。③两组不同年龄GK大鼠血管对乙酰胆碱及硝普钠的舒张反应均较Wistar大鼠显著增强。④6周龄GK大鼠血管对乙酰胆碱的舒张反应可被一氧化氮合酶(NOS)阻断剂完全阻断。而40周龄GK大鼠血管对乙酰胆碱的舒张反应不能完全被NOS阻断剂阻断,剩余的舒张部分可进一步被血红素加氧酶(HO)阻断剂阻断(P<0.01)。结论 NOS系统活性的上调可能是GK大鼠胸主动脉内皮依赖性血管舒张功能增强的主要机制,高龄GK大鼠的血管舒张功能增强可能由于NOS系统与HO系统共同参与调控所致。

EGCG对高脂饮食GK大鼠白色脂肪米色化的诱导作用与机制研究

脂肪组织类型与人体代谢密切相关,通过饮食或营养干预将白色脂肪细胞转变为产热的米色脂肪细胞是一种减少脂肪积蓄、调节代谢的安全策略。目前关于白色脂肪组织米色化作用的研究多聚焦于肥胖群体,为探究EGCG对非肥胖代谢紊乱群体的内脏白色脂肪组织米色化的诱导作用及相关机制,采用非肥胖型自发性2型糖尿病模型Goto-Kakizaki(GK)大鼠,给予每日高脂饮食,并进行40 mg·kg^(-1)和80 mg·kg^(-1)EGCG灌胃干预,检测GK大鼠的体质量、摄食量、脂肪组织细胞形态及米色化相关基因表达水平、UCP1蛋白表达水平,并进行转录组测序。结果表明,80 mg·kg^(-1)EGCG灌胃干预对GK大鼠摄食量和体质量无明显影响,但能够促使脂肪细胞呈现向多房型脂肪细胞转变趋势,并显著上调米色化相关的Pparg、Ppargc1a、Ucp1基因表达水平和UCP1蛋白表达水平,具有诱导高脂饮食GK大鼠内脏附睾白色脂肪组织米色化的作用,且表现出调节脂质代谢的潜力。结合转录组分析结果表明,EGCG对高脂饮食GK大鼠白色脂肪组织米色化的诱导作用机制可能与PPAR信号通路、PI3K/Akt信号通路和MAPK信号通路有关。

Dan-gua Fang (丹瓜方) Improves Glycolipid Metabolic Disorders by Promoting Hepatic Adenosine 5'-monophosphate Activated Protein Kinase Expression in Diabetic Goto-kakizaki Rats

Objective：To investigate the effect of Dan-gua Fang（丹瓜方） on adenosine 5’-monophosphate（AMP） activated protein kinase（AMPK） α expression in liver and subsequent improvement of glucose and lipid metabolism.Methods：Forty 13-week-old diabetic Goto-Kakizaki（GK） rats were randomly divided into model,Dan-gua Fang,metformin and simvastatin groups（n=10 for each）,and fed high-fat diet ad libitum.Ten Wistar rats were used as normal group and fed normal diet.After 24 weeks,liver expression of AMPK α mRNA was assessed by real-time PCR.AMPK α and phospho-AMPK α protein expression in liver was evaluated by Western blot.Liver histomorphology was carried out after hematoxylin-eosin staining,and blood glucose（BG）,glycosylated hemoglobin A1c（HbA1c）,food intake and body weight recorded.Results：Similar AMPK α mRNA levels were found in the Dan-gua Fang group and normal group,slightly higher than the values obtained for the remaining groups（P〈0.05）.AMPK α protein expression in the Dan-gua Fang group animals was similar to other diabetic rats,whereas phospho-AMPK α（Thr-172） protein levels were markedly higher than in the metformin group and simvastatin group（P〈0.05）,respectively.However,phosphor-AMPKa/AMPK α ratios were similar in all groups.Dan-gua Fang reduced fasting blood glucose with similar strength to metformin,and was superior in reducing cholesterol,triglycerides,high-density lipoprotein cholesterol as well as improving low-density lipoprotein cholesterol in comparison with simvastatin and metformin.Dan-gua Fang decreases plasma alanine aminotransferase（ALT） significantly.Conclusion：Dan-gua Fang,while treating phlegm-stasis,could decrease BG and lipid in type 2 diabetic GK rats fed with high-fat diet,and effectively protect liver histomorphology and function.This may be partly explained by increased AMPK expression in liver.Therefore,Dan-gua Fang might be an ideal drug for comprehensive Intervention for glucose and lipid metabolism disorders in type 2 diabetes mellitus.

Asiatic acid mitigates hyperglycemia and reduces islet fibrosis in Goto-Kakizaki rat,a spontaneous type 2 diabetic animal model

The Goto-Kakizaki(GK) rat is a spontaneous type 2 diabetic animal model,which is characterized by a progressive loss of beta islet cells with fibrosis.In the present study,the hypoglycemic effect of asiatic acid(AA) in GK rats was examined.GK rats receiving AA at a daily dose of 25 mg·kg-1 for four weeks showed a significant reduction in blood glucose levels.Age-matched normal Wistar rats were given 0.5% sodium carboxymethyl cellulose(CMC-Na) solution for the same periods and used as control.Compared to the normal Wistar rats,GK rats treated with AA showed improvement in insulin resistance partially through decreasing glucose level(P < 0.01) and insulin level(P < 0.05).Furthermore,the results of immunohistochemistry indicate that AA treatment reduced islet fibrosis in GK rats.Fibronectin,a key protein related to islet fibrosis,was over-expressed in GK rats,which was reversed significantly by AA treatment(P < 0.05).These findings suggest that AA has a beneficial effect on lowering blood glucose levels in GK rats and improves fibrosis of islets in diabetes,which may play a role in the prevention of islets

Characterization of gut microbial and metabolite alterations in faeces of Goto Kakizaki rats using metagenomic and untargeted metabolomic approach

BACKGROUND In recent years,the incidence of type 2 diabetes(T2DM)has shown a rapid growth trend.Goto Kakizaki(GK)rats are a valuable model for the study of T2DM and share common glucose metabolism features with human T2DM patients.A series of studies have indicated that T2DM is associated with the gut microbiota composition and gut metabolites.We aimed to systematically characterize the faecal gut microbes and metabolites of GK rats and analyse the relationship between glucose and insulin resistance.AIM To evaluate the gut microbial and metabolite alterations in GK rat faeces based on metagenomics and untargeted metabolomics.METHODS Ten GK rats(model group)and Wistar rats(control group)were observed for 10 wk,and various glucose-related indexes,mainly including weight,fasting blood glucose(FBG)and insulin levels,homeostasis model assessment of insulin resistance(HOMA-IR)and homeostasis model assessment ofβcell(HOMA-β)were assessed.The faecal gut microbiota was sequenced by metagenomics,and faecal metabolites were analysed by untargeted metabolomics.Multiple metabolic pathways were evaluated based on the differential metabolites identified,and the correlations between blood glucose and the gut microbiota and metabolites were analysed.RESULTS The model group displayed significant differences in weight,FBG and insulin levels,HOMA-IR and HOMA-βindexes(P<0.05,P<0.01)and a shift in the gut microbiota structure compared with the control group.The results demonstrated significantly decreased abundances of Prevotella sp.CAG:604 and Lactobacillus murinus(P<0.05)and a significantly increased abundance of Allobaculum stercoricanis(P<0.01)in the model group.A correlation analysis indicated that FBG and HOMA-IR were positively correlated with Allobaculum stercoricanis and negatively correlated with Lactobacillus murinus.An orthogonal partial least squares discriminant analysis suggested that the faecal metabolic profiles differed between the model and control groups.Fourteen potential metabolic biomarkers,including glycochenodeoxycholic acid,uric acid,13(S)-hydroxyoctadecadienoic acid(HODE),N-acetylaspartate,β-sitostenone,sphinganine,4-pyridoxic acid,and linoleic acid,were identified.Moreover,FBG and HOMA-IR were found to be positively correlated with glutathione,13(S)-HODE,uric acid,4-pyridoxic acid and allantoic acid and negatively correlated with 3-α,7-α,chenodeoxycholic acid glycine conjugate and 26-trihydroxy-5-β-cholestane(P<0.05,P<0.01).Allobaculum stercoricanis was positively correlated with linoleic acid and sphinganine(P<0.01),and 2-methyl-3-hydroxy-5-formylpyridine-4-carboxylate was negatively associated with Prevotella sp.CAG:604(P<0.01).The metabolic pathways showing the largest differences were arginine biosynthesis;primary bile acid biosynthesis;purine metabolism;linoleic acid metabolism;alanine,aspartate and glutamate metabolism;and nitrogen metabolism.CONCLUSION Metagenomics and untargeted metabolomics indicated that disordered compositions of gut microbes and metabolites may be common defects in GK rats.

RYGBP与BPD对2型糖尿病大鼠的血糖控制及GLP-1表达的影响

目的评估Roux-en-Y胃旁路术(Roux-en-Y gastric bypass,RYGBP)与胆胰分流术(billiopancreatic diver-sion,BPD)对2型糖尿病(type 2diabetes mellitus,T2DM)大鼠的临床疗效。探讨胰升糖素样多肽1(glucagon-like pep-tide 1,GLP-1)在手术治疗T2DM中的机制。方法将36只雄性正常体质量Goto-Kakizaki(GK)大鼠随机分为RYG-BP,BPD与假手术组,每组12只。观测分析非肥胖T2DM大鼠术前及术后1周、2周、1个月、2个月、3个月的体质量、空腹血糖(fasting blood glucose,FBG)、血清胰岛素(insulin,INS)水平、糖化血红蛋白(glycosylated hemoglobin A1c,HbA1c)水平、GLP-1水平的变化。观察术后3个月T2DM大鼠的并发症及死亡率的发生情况,寻找最佳手术方式。结果与术前比较,术后1周～3个月RYGBP与BPD组GK大鼠FBG显著降低(P<0.05),空腹GLP-1明显升高(P<0.05),术后3个月HbA1c显著降低(P<0.05),术后3月空腹胰岛素水平显著升高(P<0.05)。假手术组上述指标均未见明显变化。BPD组GK大鼠死亡率与并发症发生率均较RYGBP组高。结论RYGBP较BPD对非肥胖T2DM具有更安全有效的治疗作用。RYGBP控制血糖可能与GLP-1升高促进胰岛素释放,改善β细胞功能有关。

黄连解毒汤对自发性糖尿病大鼠免疫炎症因子及损伤的影响

目的:观察黄连解毒汤对自发性糖尿病大鼠心肌免疫炎症因子的影响及对心肌损伤的防治作用。方法:GK大鼠30只随机分为GK对照组、二甲双胍组、黄连解毒汤组,正常大鼠10只作为正常对照组分别灌胃12周,测定心肌匀浆核因子-κB(NF-κB)、细胞间黏附分子-1(sICAM-1)、白介素-1(IL-1)、肿瘤坏死因子(TNF-α)、内皮素-1(ET-1)含量。取心肌切片作HE染色。结果:2药物组血糖均下降(P<0.01)。GK对照组各炎症因子升高(P<0.01～0.05),黄连解毒汤组降低(P<0.01～0.05),其中NF-κB、TNF-α、ET-1与二甲双胍比较下降程度较大(P<0.01～0.05)。HE染色显示黄连解毒汤组心肌损伤明显减轻。结论:黄连解毒汤可防治糖尿病心肌炎症损伤。

梓醇对糖尿病大鼠主动脉的保护作用与抗氧化机制研究

目的:研究梓醇对Goto-Kakizaki(GK)大鼠主动脉的保护作用并探讨其抗氧化机制。方法:6月龄GK大鼠45只随机分为糖尿病模型组、二甲双胍(100 mg·kg-1·d-1)组以及梓醇高剂量(100 mg·kg-1·d-1)组、中剂量(50 mg·kg-1·d-1)组、低剂量(10 mg·kg-1·d-1)组,10只雄性Wistar大鼠作为对照组。各组灌胃给药12周,对照组和模型组给予等量的生理盐水。检测大鼠空腹血糖(FBG)和血脂;检测血清活性氧(ROS)、丙二醛(MDA)、超氧化物歧化酶(SOD)和总抗氧化力(T-AOC)水平;Western blotting检测胸主动脉组织核因子E2相关因子2(Nrf2)和血红素加氧酶1(HO-1)表达;HE染色观察胸主动脉病理变化;透射电镜观察胸主动脉组织超微结构变化。结果:梓醇治疗后,血糖和血脂显著下降;血清ROS和MDA水平明显降低,SOD活性和T-AOC显著增强;胸主动脉组织Nrf2和HO-1蛋白表达明显增强;HE染色显示胸主动脉病变程度明显减轻,透射电镜观察胸主动脉超微结构损伤明显减轻。结论:梓醇能够有效保护GK大鼠胸主动脉,其机制可能与降低血糖和血脂,减轻氧化应激反应,激活Nrf2/ARE/HO-1信号通路有关。

GK糖尿病大鼠发病机理的研究进展

自发Ⅱ型糖尿病GK大鼠与人类非肥胖型Ⅱ型糖尿病进展极为相似.GK大鼠主要特点为胰岛素分泌受损、胰岛β细胞数量减少,空腹血糖升高,肝糖原生成增多,肌肉和脂肪组织中度胰岛素抵抗等特点.文章主要从GK大鼠遗传学特征、胰腺的形态学异常及胰腺、肝脏,肌肉和脂肪组织的细胞因子的变化以及它们与Ⅱ型糖尿病的发病机理的关系的研究进展作一综述.

丹瓜方对GK糖尿病-动脉粥样硬化复合模型大鼠血糖、食量和体重的影响

目的:探讨丹瓜方对高脂饲料喂养的GK糖尿病-动脉粥样硬化复合模型大鼠血糖、食量和体重的影响。方法:40只成模GK大鼠,随机分为二甲双胍组、模型对照组、丹瓜方组、辛伐他汀组,自由进食高脂饲料,并予以相应的药物干预;另设10只同龄Wistar大鼠为正常对照组,喂食普通饲料;观察大鼠血糖、HbA1c、体重、食量的变化情况。结果:丹瓜方组血糖与空白对照组比较无差异,且优于其他各模型组;丹瓜方组HbA1c与二甲双胍组比较无差别,且低于模型对照组(P<0.05);GK大鼠食量均明显减少,丹瓜方组食量低于空白对照组和模型对照组(P<0.01);GK大鼠体重均低于空白对照组,丹瓜方组体重增幅最小(P<0.05)。结论:丹瓜方在控制高脂饲料喂养的GK大鼠的血糖、体重和食量上具有明显优势。

胃旁路术对非肥胖2型糖尿病GK大鼠的降糖作用

目的:观察胃旁路术(gastric bypass,GBP)对非肥胖型2型糖尿病GK大鼠(Goto-Kakizaki rats)的降糖作用及其机制。方法:雄性GK大鼠和SD大鼠各20只,随机分为GK手术组、GK假手术组、SD手术组、SD假手术组,每组10只。测定术前及术后第1、2、4、8周各组体重、空腹血糖(FPG)、糖耐量(OGTT)、血浆胰岛素(INS)、血浆胰高血糖素样肽-1(GLP-1)水平。结果:术后8周,GK手术组FPG和OGTT由术前的(5.0500±0.395)mmol/L和(22.7900±3.525)mmol/L下降到(4.0125±0.476)mmol/L和(12.4875±1.173)mmol/L,血浆INS和GLP-1由术前的(674.00±224.372)pg/mL和(6915.00±1566.860)pg/mL上升到(873.63±115.920)pg/mL和(8508.75±1247.013)pg/mL,差异均有显著性(P<0.05)。结论:GBP能显著改善非肥胖型2型糖尿病GK大鼠糖代谢,与术后肠胰岛轴改变血浆INS、GLP-1水平升高有关。

2型糖尿病大鼠主动脉硬化模型的构建

目的:建立自发2型糖尿病大鼠主动脉硬化动物模型。方法:用2型糖尿病大鼠主动脉硬化动物模型。44只GK大鼠随机分为正常GK对照组、建模组,每组22只,正常Wistar大鼠组22只。期间观察大鼠血糖、尿糖及一般情况变化,8周后,测定各组动物空腹血糖、总胆固醇(total cholesterol,TC)、甘油三酯(triglycerides,TG)、低密度脂蛋白胆固醇(low density lipoprotein choleste rol,LDL-C),同时光学显微镜观察主动脉结构。结果:模型组大鼠的总胆固醇、甘油三酯、低密度脂蛋白胆固醇明显升高,出现主动脉肥大,病理显示明显的主动脉及动脉内膜病变。结论:通过高脂、一氧化氮合成酶抑制剂,可成功构建自发2型糖尿病大鼠主动脉病变,用作2型糖尿病大鼠大血管病变研究的动物模型。

黄芪调节自发糖尿病肾病鼠层粘连蛋白表达的实验研究

目的:观察黄芪对自发糖尿病肾病大鼠肾小球层粘连蛋白表达的影响。方法:将实验用6月龄SPF级GK大鼠和Wistar大鼠随机分为正常对照组、糖尿病组、黄芪治疗组。治疗16周,观察治疗后大鼠的尿素氮、血肌苷,内生肌苷清除率、24小时尿蛋白排泄率,免疫组化检测肾组织层粘连蛋白表达。结果:造模组大鼠均出现肾脏功能有损害。黄芪能改善自发糖尿病肾病大鼠基本状况,降低糖尿病大鼠的尿素氮、血肌苷、24h尿白蛋白排泄率,增加内生肌苷清除率,层粘连蛋白表达显著下调。结论:黄芪可通过降低层粘连蛋白的表达,对肾脏起保护作用。

自发性糖尿病GK大鼠糖尿病周围神经病变模型的建立

目的通过高脂饲养GK大鼠建立一种符合人类糖尿病周围神经病变（DPN）发病特点，又操作简单的DPN大鼠模型。方法7~8周龄SPF级雄性自发性2型糖尿病GK大鼠30只，喂养高脂饲料造模。另取30只SPF级正常Wistar大鼠作为正常组，喂养普通饲料。每周监测动物血糖、体质量、饮水量、饲料量。分别于干预8周、12周、16周后检测血清糖化血红蛋白、坐骨神经传导速度，取对侧坐骨神经做HE染色，TUNEL染色计算细胞凋亡指数。结果随着造模时间延长，GK大鼠逐渐出现多饮、多食、生长迟缓等表现。与正常组相比，造模12周及16周的大鼠血糖、糖化血红蛋白升高（P<0.01），感觉神经传导速度降低（P<0.01），运动神经传导速度有一定下降趋势（12周P<0.05，16周P>0.05），坐骨神经病理形态及雪旺细胞凋亡情况均提示DPN的形成，并与正常大鼠形成鲜明对照（凋亡指数P<0.01）。结论长期高脂饲料喂养的GK大鼠是DPN研究的良好模型，12周是较为成熟且经济的造模时间。

沙蓬粗寡糖对GK大鼠胰岛素抵抗的影响

目的观察沙蓬粗寡糖(AOS)对糖尿病GK大鼠降血糖、改善胰岛素抵抗作用,探讨可能机制。方法将符合2型糖尿病GK大鼠随机分为模型对照组(MC)、格列苯脲组(GLB)、沙蓬粗寡糖高(AOS-H)、中(AOS-M)、低剂量组(AOS-L),以同源Wistar大鼠为正常对照(NC)。各组均灌胃给药8周,测定给药前后空腹血糖(FBG)、随机血糖(RBG)、糖耐量(OGTT);给药8周测定非空腹非糖负荷状态的给药前后血糖及血清胰岛素含量变化;结束时测空腹血清血糖(FPG)、胰岛素(FINS)、OGTT,计算胰岛素抵抗指数(HOMA-IR);取胰腺常规石蜡包埋,HE染色,观察其病理组织形态改变。结果 AOS对GK大鼠空腹血糖影响不明显,但明显降低随机血糖,改善糖耐量,增加胰岛素敏感性,且明显减小AUC(P<0.01),以中剂量效果更好,与格列苯脲相似;AOS能促进胰岛素释放,以AOS中、低剂量促胰岛素释放作用更强,在释放时间和释放量上均早于和强于格列本脲;AOS可抑制GK大鼠胰岛组织病理改变,增加胰岛及胰岛细胞数量,与模型组比较,AOS给药组胰岛组织结构改变明显减轻。结论 AOS具有明显改善胰岛素抵抗和降低血糖作用,其机制可能是与快速促进胰岛素释放,增加胰岛细胞增值,改善胰岛功能有关。