新型肝X受体激动剂ATI-829对糖尿病小鼠的治疗作用

J4 ›› 2012, Vol. 38 ›› Issue (3): 443-446.

新型肝X受体激动剂ATI-829对糖尿病小鼠的治疗作用

彭璐¹|赵兴山¹|谢景田²|彭大成²|兰玲³

（1.北京积水潭医院心血管内科|北京 100035；2.芝加哥大学医学院Ben |May研究中心|美国　芝加哥 |60637；3.北京积水潭医院内分泌科|北京 |100035）

收稿日期:2012-01-11 出版日期:2012-05-28 发布日期:2012-05-28
通讯作者: 兰玲 E-mail:（Tel: 010-58516688，E-mail: lupeng11@163.com）
作者简介:彭璐 (1974-)|女|北京市人|主治医师|医学硕士|主要从事代谢疾病的基础及临床研究。
基金资助:
国家自然科学基金资助课题（30901725）

Effect of |novel liver X receptor agonist ATI-829 in |treatment of diabetic mice

PENG |Lu¹,ZHAO Xing-shan¹,XIE Jing-tian²,PENG Da-cheng²,LAN Ling³

(1.Department of |Cardiology,Beijing Jishuitan Hospital,Beijing 100035,China|2.Ben May Research Center,School of Medical Science,Chicago University,Chicago 60637,USA|3.Department of |Endocrinology,Beijing Jishuitan Hospital,Beijing 100035,China)

Received:2012-01-11 Online:2012-05-28 Published:2012-05-28

摘要/Abstract

摘要：

目的: 观察新型肝X受体激动剂ATI-829对2型糖尿病KKAy小鼠的血糖、体质量和摄食量及NOD小鼠1型糖尿病发生率的影响，为ATI-829的临床应用提供依据。方法: 将15只12周龄雄性KKAy 2型糖尿病小鼠分为溶媒对照组、吡格列酮治疗组和ATI-829治疗组。每周进行1次血糖、体质量和摄食量的监测，共给药2周。40只6周龄的雌性1型糖尿病NOD小鼠分为溶媒对照组、传统肝X受体激动剂T1317治疗组和ATI-829治疗组，共给药8周，从小鼠20周龄起，每2周监测1次血糖水平，持续监测至34周龄。结果:在KKAy2型糖尿病小鼠实验中，治疗1周后，各组小鼠血糖水平、体质量和摄食量变化与治疗前比较差异均无统计学意义(P<0.05)。治疗2周后吡格列酮治疗组血糖浓度由(30.11±3.94) mmol.L^-1降至(14.00±2.78) mmol.L^-1，小鼠体质量由(36.96±1.17) g升高到(41.14±0.99) g，与溶媒对照组比较差异均有统计学意义（P<0.05）。ATI-829治疗组血糖浓度由(33.28±1.89) mmol.L^-1降至(15.89±1.06) mmol.L^-1，与溶媒对照组比较差异有统计学意义（P<0.05），小鼠体质量由(37.82± 0.96) g降至(37.11±0.26) g，但与溶媒对照组比较差异无统计学意义（P> 0.05）。吡格列酮和ATI-829均不影响小鼠摄食量。在1型糖尿病NOD小鼠实验中，溶媒对照组最终小鼠糖尿病发病率为50%，T1317治疗组发病率达90%，而ATI-829 治疗组无小鼠发病，T1317组和ATI-829治疗组发病率与溶媒对照组比较差异均有统计学意义（P<0.05）。结论: 新型肝X受体激动剂ATI-829能有效降低2型糖尿病小鼠血糖浓度，且不诱导其体质量增加，同时亦可降低小鼠1型糖尿病的发生率。

关键词: 肝X受体；激动剂；糖尿病

Abstract:

To observe the influence of novel liver X receptor (LXR) agonist ATI-829 on the blood glucose level,body weight and dietary consumption of type 2 diabetes mellitus KKAy mice and the incidence of type 1 diabetic NOD mice, and to provide evidence for clinical application.Methods Fifteen 12-week male type 2 diabetes mellitus KKAy mice were randomly divided into vehicle control group,pioglitazone treatment group,and ATI-829 treatment group.The mice were treated for 2 weeks, and the blood glucose levels,body weights,and the dietary consumptions of mice were measured every week.Forty 6-week female type 1 diabetes mellitus NOD mice were divided into vehicle control group,classic LXR agonist T1317 treatment group,and ATI-829 treatment group.The mice were treated for 8 weeks, and the cumulative incidence was measured every two weeks from 20 to 34 week.Results In type 2 diabetes mellitus mice,after 1 week treatment,the glucose level,body wieght and the dietry consumption of mice in various groups didn’t change significantly compared with those before treatment.After 2 weeks treatment, the blood glucose level of mice in pioglitazone treatment group was decreased from (30.11±3.94) mmol.L^-1 to (14.00±2.78) mmol.L^-1,and the body weight was increased from (36.96±1.17) g to (41.14±0.99) g,there were significant differences compared with vehicle control group(P<0.05).The blood glucose level of mice in ATI-829 treatment group was decreased from(33.28±1.89) mmol.L^-1 to (15.89±1.06) mmol.L^-1,there was significant difference compared with vehicle control group(P<0.05);and the body weight was decreased from (37.82±0.96) g to (37.11±0.26) g,there was no significant difference compared with vehicle control group(P>0.05).The dietary consumption didn’t change significantly in various groups before and after treatment.In type 1 diabetic NOD mice,ATI-829 was able to totally prevent the disease occurrence and the disease incidence in T1317 treatment group rose to 90%,which was 50% in vehicle control group，there were significant differences between T1317 group,ATI-829 treatment group and vehicle control group(P<0.05).Conclusion The novel liver X receptor agonist ATI-829 can decrease the blood glucose levels of type 2 diabetes mellitus mice and avoid body weight gain.Meanwhile,ATI-829 can also decrease the incidence of type 1 diabetes mellitus in mice.

中图分类号:

R587.1

彭璐|赵兴山|谢景田|彭大成|兰玲. 新型肝X受体激动剂ATI-829对糖尿病小鼠的治疗作用[J]. J4, 2012, 38(3): 443-446.

PENG Lu,ZHAO Xing-shan,XIE Jing-tian,PENG Da-cheng,LAN Ling. Effect of |novel liver X receptor agonist ATI-829 in |treatment of diabetic mice[J]. J4, 2012, 38(3): 443-446.

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