交泰丸对2型糖尿病大鼠胰岛形态的影响

目的:研究交泰丸对2型糖尿病大鼠胰岛形态的影响。方法:用高糖高脂饲料喂养大鼠6周,腹腔注射低剂量链脲佐菌素(STZ)37mg/kg制作大鼠2型糖尿病动物模型。给予交泰丸水煎剂灌胃治疗5周,动态观察其治疗后的饮水量、进食量、体重、空腹血糖(FBG)变化,于治疗5周后检测血清游离脂肪酸(FFA)、甘油三酯(TG)、血清胰岛素(INS)水平;并取胰腺在光镜和透射电子显微镜下观察组织形态学变化;免疫组化法观察胰岛素阳性细胞。结果:与模型组比较,交泰丸组在用药1周末即出现FBG降低趋势,5周末有明显差异;3周后进食量明显减少;TG、FFA与模型组比较显著下降;组织形态学观察胰岛结构较完整,细胞数量相对增多,细胞内分泌颗粒较丰富,胰岛周边部导管上皮细胞样细胞增多,并向胰岛中央移行;免疫组化结果显示,交泰丸组胰岛内胰岛素阳性细胞较多,染色较深。结论:交泰丸对2型糖尿病大鼠胰岛结构具有保护作用。

1,6-二磷酸果糖对白细胞介素1β损伤的胰岛细胞功能的影响

目的:应用离体培养乳鼠胰岛细胞,探讨1,6-二磷酸果糖(fructose-1,6-diphosphate,FDP)对白细胞介素1β(IL-1β)损伤的胰岛细胞是否具有保护作用。方法:实验选用出生1～3d的Wistar大鼠20只。分离培养后的胰岛细胞,将其随机分为对照组、FDP组、IL-1β损伤组、IL-1β+FDP组,每组平行孔为6孔。应用MTT法检测对照组、IL-1β损伤组以及不同浓度(2.5,5.0,7.5,10.0,12.5,15.0mmol/L)FDP保护组胰岛细胞的细胞活性。结果:IL-1β损伤组细胞活性(A值:0.116±0.012)明显低于对照组(0.252±0.020)(F=8.92,P<0.01),加入5～10mmol/LFDP可使细胞活性增强(F=13.35,22.56,P<0.01),但2.5,12.5,15.0mmol/LFDP与受损细胞共同孵育后未能使细胞活性升高(P>0.05)。10,40h时未见FDP对受损细胞活性的保护,20h时IL-1β+FDP组细胞活性(A值:0.219±0.004)明显高于IL-1β损伤组(0.178±0.010)(F=19.10,P<0.01),30hIL-1β+FDP组细胞活性明显高于IL-1β损伤组(F=16.05,P<0.01)。结论:FDP对IL-1β损伤的胰岛细胞活性具有保护作用,且具有时间和剂量依从关系。

结肠癌合并2型糖尿病患者胰岛素样生长因子-I表达与淋巴结转移的关系

[目的]探讨结肠癌合并2型糖尿病（T2DM）患者胰岛素样生长因子-I（IGF-I）表达与淋巴结转移的关系.[方法]采用免疫组织化学方法检测38例结肠癌合并T2DM患者和单纯结肠癌患者结肠癌组织中IGF-I表达情况.[结果]结肠癌合并T2DM患者组IGF-I阳性表达率（71.43%）明显高于无糖尿病组（DM）（47.22%）（ P 〈0.05）.有淋巴结转移者占IGF-I阳性表达者中60.6%（20/33）,显著高于IGF-I阴性表达中有淋巴结转移者的比例（37.5%,9/24）.[结论]T2DM可能增加结肠癌淋巴结转移几率.

不同HIV蛋白酶抑制剂对鼠胰岛素瘤细胞功能的影响

目的:探讨不同H IV蛋白酶抑制剂对胰岛beta-细胞功能的影响。方法:体外观察不同浓度ritonav ir或am prenav ir干预48 h对鼠胰岛素瘤IN S-1细胞葡萄糖刺激的胰岛素释放速率的影响,胰岛素测定采用EL ISA法,并用细胞内DNA含量标准化。用苔盘蓝染色细胞计数、MTT试验评估ritonav ir或am prenav ir对IN S-1细胞活力的影响。结果:R itonav ir治疗可以显著降低基础胰岛素分泌速率及葡萄糖刺激的胰岛素释放速率,并呈剂量依赖关系(r分别为-0.861,-0.839,均P<0.01)。10μm o l/L ritonav ir分别降低基础胰岛素分泌和葡萄糖刺激的胰岛素释放达46%和47%。Am prenav ir对胰岛素释放功能没有影响。结论:不同H IV蛋白酶抑制剂对胰岛beta-细胞功能的影响不同。

冠心病中医辨证分型的临床研究

20世纪70年代起我国即开展了冠心病(CHD)中医辨证分型的研究,结合现代医学的客观化指标和量化手段,在中医辨证分型和证型客观化方面均取得了丰硕成果。研究显示,冠心病中医证型与血液流变学、血脂、胰岛素抵抗、冠脉造影、细胞因子关系密切,从而为中医辨证论治体系的规范化、客观化提供了依据,也提高了中医诊治CHD的临床疗效。

LINK BETWEEN OXIDATIVE STRESS AND INSULIN RESISTANCE

Many studies on oxidative stress,insulin resistance,and antioxidant treatment have shown that increased oxidative stress may accelerate the development of diabetic complications through the excessive glucose and free fatty acids metabolism in diabetic and insulin-resistant states.Many pathogenic mechanisms such as insulin receptor substrate phosphorylation are involved in insulin resistance induced by oxidative stress.And antioxidant treatments can show benefits in animal models of diabetes mellitus and insulin resistance.However,negative evidence from large clinical trials suggests that new and more powerful antioxidants need to be studied to demonstrate whether antioxidants can be effective in treating diabetic complications.Furthermore,it appears that oxidative stress is only one of the factors contributing to diabetic complications.Thus,antioxidant treatment would most likely be more effective if it were coupled with other treatments for diabetic complications.

CLINICOPATHOLOGIC FEATURES AND SURGICAL TREATMENT OF NONFUNCTIONING ISLET CELL TUMORS

Objective.To in vestigate clinicopathologic characteristics and surgical results of nonfunctiona l islet cell tumors.Methods.We performed retrospective analysis of50patient s with nonfunctional islet cell tumor treat-ed at Peking Union Medical College Hospital from July1968to July1999,and summarized clinical symptoms and signs,primary diagnosis before surgery,surgical treatments,pathologic and im munohisto-logical characteristics.Results.Of the50cases examined from July 1968to July1999,12were found during physical examinations. The most common symptoms were upper abdominal pain and upper abdominal dis-com fort,which appeared in20casesand17casesrespectively,an d the most common sign was abdominal masses.B-ultrasound and CT are the most commonly used means for preoperative examination,with posit ive rates of97.8%and100%respectively.Op-e rative mortality was2%.Five-year survival rate of radical surgery of maligna nt cases was75%.Immuno-histological examinations showed that tumors rich i n multi-peptide linked hormones,neuron-specific eno-lase and chromaffin were in65%cases,90.6%and73.3% respectively.The positive rates of insulin,glucagons,somatostatin,pancreat ic polypeptide,gastrin and vasoactive intestinal peptide were68.2% ,51.2%,42.9%,40% ,25%and15.8%respectively.Conclusion.Nonfuncti onal islet cell tumors lack diagnostic specificity.Ultrasound and CT are primar y examination methods.Immunohistological analysis indicates different hormones ,but lacks the presence of related clinical symptoms.Surgery is an effective treatment for nonfunctional islet cell tumors,and even for those with distal m etastasis,immediate surgical removal and treatment can improve prognosis.

An inherent acceleratory effect of insulin on small intestinal transit and its pharmacological characterization in normal mice

AIM： To study an inherent effect of insulin on small intestinal transit and to explore involvement of various systems/mechanisms in normal mice. METHODS： Insulin at the doses of 2 μU/kg, 2 mU/kg, 2 U/kg or vehicle was subcutaneously administered to four groups of overnight fasted normal male mice. Blood glucose （BG） levels were measured 2 min before insulin administration and 2 min before sacrificing the animals for the measurement of small intestinal transit （SIT）. Charcoal meal was administered （0.3 mL） intragastrically 20 min after insulin administration and animals were sacrificed after 20 min and SIT was determined. For exploration of the various mechanisms involved in insulin-induced effect on SIT, the dose of insulin which can produce a significant acceleration of SIT without altering BG levels was determined. The following drugs, atropine （1 mg/kg）, clonidine （0.1 mg/kg）, ondansetron （1 mg/kg）, naloxone （5 mg/kg）, verapamil （8 mg/kg） and glibenclamide （10 mg/kg）, were administered intravenously 10 min prior to the administration of insulin （2 μU/kg）. RESULTS： The lower doses of insulin （2 μU/kg and 2 mU/kg） produced a significant acceleration of SIT from 52.0% to 70.7% and 73.5% without lowering blood glucose levels （P〈0.01）, while the highest dose of insulin （2 U/kg） produced a fall in blood glucose levels which was also associated with significant acceleration of SIT （P〈0.01）. After pretreatment of insulin （2 μU/kg） group with atropine, insulin could reverse 50% of the inhibition produced by atropine. In clonidine-pretreated group, insulin administration could reverse only 37% of the inhibition produced by clonidine and inhibition of SIT was significant compared with vehicle ＋ insulintreated group, i.e. from 74.7% to 27.7% （P〈0.01）. In ondansetron-pretreated group, insulin administration could produce only mild acceleration of SIT （23.5%）. In naloxone-pretreated group, insulin administration could significantly reverse the inhibition of SIT produced by naloxone when compared with naloxoneperse group, i.e. from 32.3% to 53.9% （P〈0.01）. In verapamil-pretreated group, insulin administration could only partially reverse the inhibition （65%）. In glibenclamide-pretreated group, insulin administration produced further acceleration of SIT （12.2%）. CONCLUSION： Insulin inherently possesses an acceleratory effect on SIT in normal mice. Adrenergic and cholinergic systems can play a significant role. Calcium channels and opioidergic system can play a supportive role; in addition, enhancement of endogenous insulin release can augment the effect of exogenously administered insulin on SIT.

FoxO1因子与β细胞去分化的关系

2型糖尿病是由于β细胞功能缺陷导致不同程度的胰岛素缺乏和组织胰岛素抵抗的慢性代谢性疾病.β细胞功能下降是2型糖尿病进展的中心环节,而胰岛β细胞去分化作为胰岛功能减退的重要机制之一,近年有研究显示,叉头转录因子O亚组1(FoxO1)活性下降与β细胞去分化密切相关.研究FoxO1参与β细胞去分化的具体发生机制并促进去分化的β细胞再分化将会为2型糖尿病的预防和治疗提供新的思路.