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MKR转基因小鼠糖尿病发病特点的初步探讨
引用本文:喻嵘,成细华,胡伟,魏开春.MKR转基因小鼠糖尿病发病特点的初步探讨[J].实验动物与比较医学,2007(5):333-337.
作者姓名:喻嵘  成细华  胡伟  魏开春
作者单位:湖南中医药大学科技处 长沙410007
基金项目:国家自然科学基金;国家中医药管理局回国留学人员项目;湖南省教育厅资助项目;湖南省科技厅科技计划
摘    要:目的观察骨骼肌胰岛素样生长因子-1受体及胰岛素受体的功能缺失(Mouse overexpressing adominant-negative IGF-I receptor specifically in muscle,MKR mouse)转基因2型糖尿病小鼠的血糖及其生长情况。方法由美国国立卫生研究院(NIH)授权使用引进的MKR鼠,经自然交配后繁殖的子代作为研究对象,制备尾组织基因组DNA,经聚合酶链反应得到扩增产物,1%琼脂糖凝胶电泳观察鉴定。同时对MKR鼠子代出生后的血糖、体重、胰岛素定时检测。同期采用昆明种小鼠或C57野生型小鼠进行对照。结果MKR鼠所有子代鼠均会出现长度为330 bp的DNA片段,表明该MKR鼠后代能稳定遗传。新生MKR鼠自出生3周开始,即出现显著的血糖增高,5周以后血糖则较稳定地维持在高水平。与对照组小鼠同期的血糖比较,差异具有非常显著性意义(P<0.01)。其体重增长随年龄的增长而减慢,至4月龄时体重基本稳定,但无下降趋势。MKR鼠在2月龄时即表现出显著的高胰岛素血症及糖耐量低下,与对照组小鼠同期比较,亦具有非常显著性意义(P<0.01)。MKR鼠在生长过程中无自然死亡发生。结论MKR鼠是至今为止一种非常良好的2型糖尿病的动物模型。

关 键 词:2型糖尿病  小鼠  转基因技术  胰岛素样生长因子-1受体  胰岛素受体
修稿时间:2007/4/10 0:00:00

Diabetic Characteristics of MKR Mice with Skeletal Muscle-Specific Double Deficiency of IGF-I and Insulin Receptors
Yubin Guo,Jun-Li Liu,YU Rong,CHENG Xi-hu,HU Wei,WEI Kai-chun,Yubin Guo,Jun-Li Liu.Diabetic Characteristics of MKR Mice with Skeletal Muscle-Specific Double Deficiency of IGF-I and Insulin Receptors[J].Laboratory Animal and Comparative Medicine,2007(5):333-337.
Authors:Yubin Guo  Jun-Li Liu  YU Rong  CHENG Xi-hu  HU Wei  WEI Kai-chun  Yubin Guo  Jun-Li Liu
Abstract:Objective To develop a diabetic mouse model to investigate metabolic changes of blood glucose level and body weight in the MKR mouse,a model in which expression of a dominant-negative IGF-I receptor in the skeletal muscle leads to systemic insulin resistance and diabetes.Methods\ MKR mice were received from the National Institutes of Health,USA,and genotyped by a specific PCR reaction using tail DNA.These mice were followed up for blood glucose level and body weight once a week from 1 to 16 weeks of age.The serum insulin level and glucose tolerance were determined at two months,using wild-type Kunming mice or C57 mice as controls.Results\ The offspring of MKR mice exhibited stable transgenic hereditary.These mice were hyperglycaemic from 3 weeks of age onward.The body weight increase slowed down after 4 month.There was 20-fold hyperinsulinemia in MKR vs.wild-type littermates,and very significant glucose intolerance in 2month-old MKR mice.The hyperglycemia is more severe in male especially older male MKR mice,than their female counterparts.Conclusion\ We have estabolished the MKR model,set up a PCR reaction to genotype and revealed sexual dimorphic changes in the type 2 diabetes.
Keywords:Type 2 diabetes  Mouse  Transgenic technology  Insulin-like growth factor 1 receptor  Insulin receptor
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