UCP1和UCP3基因表达减少与OLETF鼠早期肥胖有关

基础医学与临床 ›› 2011, Vol. 31 ›› Issue (3): 286-290.

UCP1和UCP3基因表达减少与OLETF鼠早期肥胖有关

金成吉¹,王晓梅¹,李湘¹,李湘¹,母义明²,母义明²

1. 大连大学附属中山医院
2. 中国人民解放军总医院内分泌科

收稿日期:2009-11-02 修回日期:2010-07-20 出版日期:2011-03-05 发布日期:2011-03-14
通讯作者: 金成吉 E-mail:jinchj68@yahoo.com.cn

UCP1 and UCP3 play an important role in the early stage of the development of obesity in OLETF rats

JIN Cheng-ji ¹,WANG Xiao-mei ²,LI Xiang ²,LI Xiang ²,MU Yi-ming ²,MU Yi-ming ²

1. ZhongShan Hospital Affiliated to DaLian Univesity
2.

Received:2009-11-02 Revised:2010-07-20 Online:2011-03-05 Published:2011-03-14
Contact: JIN Cheng-ji E-mail:jinchj68@yahoo.com.cn

摘要/Abstract

摘要： 目的观察肥胖2型糖尿病模型OLETF鼠体质量变化和解偶联蛋白（UCPs）转录基因或蛋白表达的相关性。方法测量OLETF大鼠和对照组LETO大鼠不同周龄阶段体质量，在7、10和25周时用Western方法测定棕色脂肪组织（BAT）中的UCP1蛋白，用Northern方法测定骨骼肌中UCP2和UCP3 mRNA量。结果 OLETF大鼠体质量增加比LETO大鼠快，9周前后两组体质量增加差异最明显。10周时LETO组UCP1 是OLETF组的1.9倍（p<0.05）； UCP3 mRNA量约为OLETF的5.5倍(p<0.01)。结论体重增加差异明显的阶段UCP1和UCP3基因表达的减少可能是引起OLETF大鼠肥胖的病因之一。

关键词: 肥胖, UCP1, UCP2, UCP3

Abstract: Objective To investigate the relationship between the body weight change and the mRNA or protein expression of uncoupling proteins (UCPs) in OLETF rats. Methods Body weights were measured per weeks. UCP1 protein expression in the brown adipose tissue was detected by western blotting, while UCP2, UCP3 mRNA expression in the skeletal muscle was measured by northern hybridization in the OLETF and LETO rats at age of 7,10 and 25 weeks. Results OLETF rats gained weight at a faster rate than LETO rats, and the difference in the rate of weight gain was most prominent around 9 weeks of age. UCP1 protein level was 1.9-fold higher in LETO than OLETF rats at 10 weeks of age (p<0.05). UCP3 mRNA level was 5.5-fold higher in LETO than OLETF rats at 10 weeks of age (p<0.01). Conclusions: UCP1 and UCP3 expression may play an important role particularly in the early stage of the development of obesity in OLETF rats.

中图分类号:

金成吉王晓梅李湘李湘母义明母义明. UCP1和UCP3基因表达减少与OLETF鼠早期肥胖有关 [J]. 基础医学与临床, 2011, 31(3): 286-290.

JIN Cheng-ji WANG Xiao-mei LI Xiang LI Xiang MU Yi-ming MU Yi-ming. UCP1 and UCP3 play an important role in the early stage of the development of obesity in OLETF rats[J]. Basic & Clinical Medicine, 2011, 31(3): 286-290.

[1]	王珺怡朱建强贾德政袁新帕孜丽耶·亚森关亚群梁小弟. 抗小鼠移码因子1蛋白多抗制备及其在脂肪细胞分化中的表达[J]. 基础医学与临床, 2018, 38(3): 335-339.
[2]	彭茜安振梅. 运动防治肥胖的分子机制[J]. 基础医学与临床, 2014, 34(5): 715-718.
[3]	张华边德志张梅班博. BRL37344增强3T3-L1前体脂肪细胞[J]. 基础医学与临床, 2013, 33(7): 908-909.
[4]	王永玲高建芝李冬霞李绍山. 血管内皮细胞生长因子在肥胖乳腺癌患者乳腺癌组织中的表达及临床意义[J]. 基础医学与临床, 2012, 32(5): 544-547.
[5]	徐铖杨啸林朱广瑾张正国. 黑龙江省成人不同肥胖类型与心室复极不一致性的关系[J]. 基础医学与临床, 2010, 30(6): 582-586.
[6]	李艳梅姚树坤. 摄食的外周调节信号[J]. 基础医学与临床, 2010, 30(11): 1234-1237.
[7]	梁晓燕卢慧玲胡秀芬吴静. 促酰化蛋白通过PLC信号途径调控脂滴相关蛋白TIP47的表达[J]. 基础医学与临床, 2009, 29(9): 897-900.
[8]	焦谊刘晓宇王延蛟张成艾克拜尔.艾力关亚群. 新疆维吾尔族肥胖患者网膜脂肪组织脂联素mRNA表达降低[J]. 基础医学与临床, 2009, 29(6): 647-648.
[9]	郭真袁良杰卢霞蔺美玲郑天珍李伟. 厚朴酚对高脂饮食性肥胖大鼠体重及胰岛素抵抗的影响[J]. 基础医学与临床, 2008, 28(9): 936-939.
[10]	鲁瑾邹大进. 肥胖人群中瘦素受体基因Lys656Asn多态性与血三酰甘油水平的相关性[J]. 基础医学与临床, 2008, 28(3): 252-255.
[11]	车建华李玄关咏梅. 多囊卵巢综合征患者血PAI-1和uPA含量的变化[J]. 基础医学与临床, 2008, 28(1): 31-34.
[12]	姚树坤柯美云王智凤. 逆行胃电刺激对健康人饮水、摄食和胃排空的影响[J]. 基础医学与临床, 2006, 26(5): 513-517.