大黄素对高糖环境下系膜细胞收缩功能的影响

山东大学学报(医学版) ›› 2010, Vol. 48 ›› Issue (9): 14-18.

大黄素对高糖环境下系膜细胞收缩功能的影响

刘友霞1，刘毅2，曹铭锋1，完强1，王群1，王荣1

山东大学附属省立医院 1.肾内科； 2.呼吸内科，济南 250021

收稿日期:2009-12-23 出版日期:2010-09-16 发布日期:2010-09-16
通讯作者: 王荣（1965- ），男，主任医师，主要从事肾脏病与血液净化的研究。 E-mail ：wangrong2@medmail.com.cn
作者简介:刘友霞（1987- ），女，硕士研究生，主要从事肾脏病与血液净化的研究。
基金资助:
国家自然科学基金资助项目（30971381）；山东省博士基金资助项目（2006BSB14022, 2003BS059）；山东省自然科学青年基金资助项目（Q2006C15）。

Emodin ameliorates high-glucose-induced mesangial cell hypocontractility

LIU You-xia1, LIU Yi2, CAO Ming-feng1, WAN Qiang1, WANG Qun1, WANG Rong1

1. Department of Nephrology; 2. Department of Respiratory Diseases, Provincial Hospital Affiliated to Shandong University, Jinan 250021, China

Received:2009-12-23 Online:2010-09-16 Published:2010-09-16

摘要/Abstract

摘要：

目的探讨高糖环境下大黄素能否通过抑制系膜区p38丝裂原活化蛋白激酶(p38MAPK)的过度活化而改善系膜细胞的收缩功能。方法培养系膜细胞，调整培养液为以下5组：正常糖组（糖浓度5.6mmol/L，NG组）、高糖组（糖浓度30mmol/L，HG组）、低质量浓度大黄素组（50mg/L大黄素+高糖，LE组）、高质量浓度大黄素组（100mg/L大黄素+高糖，HE组）和过氧化物酶体增殖物活化受体γ（PPARγ）抑制剂GW9662组（10μmol/L GW9662+高糖+高质量浓度大黄素，GW组）。系膜细胞收缩力以细胞收缩前后表面积的变化表示，采用Western blot和Realtime PCR法测定p38MAPK的活性及PPARγ的表达水平。结果高糖组p38 MAPK的活性增加，系膜收缩功能明显下降（P<0.05）；大黄素组能明显抑制p38MAPK的过度活化进而改善系膜细胞的收缩功能，且具有剂量依赖性（50mg/L大黄素组p38活性降低了40%，100mg/L组降低了73%，P均<0.05）；大黄素组PPARγmRNA水平及其蛋白水平均明显升高（P均<0.05）；PPARγ抑制剂GW9662能有效地阻断大黄素所产生的保护效应（P<0.05）。结论高糖环境下，大黄素通过激活PPARγ抑制系膜区p38MAPK的过度活化进而改善系膜细胞的收缩功能。

关键词: 大黄素；高糖；系膜细胞；p38丝裂原活化蛋白激酶；过氧化物酶体增殖物活化受体γ

Abstract:

Objective To explore whether emodin ameliorates high-glucose-induced mesangial cell hypo-contractility by inhibiting p38MAPK over-activation. Methods Mesangial cells were divided into five groups： the normal glucose group (5.6mmol/L glucose, NG group), the high glucose group (30mmol/L glucose, HG group), the low-dose emodin group (50mg/L emodin+ 30mmol/L glucose， LE group), the high-dose emodin group (100mg/L emodin+30mmol/L glucose, HE group), and the GW9662 group (10μmol/L GW9662+ 30mmol/L glucose+100mg/L emodin, GW group). Angiotensin Ⅱ-stimulated cell surface reduction was measured to evaluate cell contractility. p38MAPK activity and PPARγ expression were detected by using Western blot and real-time polymerase chain reaction(Real-time PCR). Results High-glucose resulted in an increase in p38MAPK activity and significant impairment of mesangial contractility（P<0.05）; emodin treatment dose-dependently inhibited high-glucose-induced p38MAPK overactivation(a 40% decrease for 50mg/L emodin and a 73% decrease for 100 mg/L emodin), and mesangial hypo-contractility was ameliorated by emodin（P<0.05）; both the PPARγ mRNA and protein levels were elevated after emodin treatment（P<0.05）; inhibition of PPARγ using GW9662 effectively blocked ameliorating effects of emodin on high-glucose-induced p38MAPK over-activation and mesangial hypo-contractility（P<0.05）. Conclusion Emodin effectively ameliorates high-glucose-induced p38MAPK over- activation via activation of PPARγ, and therefore, ameliorateshypo-contractility of mesangial cells.

Key words: Emodin; High glucose; Mesangial cells; p38 mitogen-activated protein kinases; Peroxisome proliferator activated receptors gamma

中图分类号:

R285.5

刘友霞1，刘毅2，曹铭锋1，完强1，王群1，王荣1. 大黄素对高糖环境下系膜细胞收缩功能的影响[J]. 山东大学学报(医学版), 2010, 48(9): 14-18.

LIU You-xia1, LIU Yi2, CAO Ming-feng1, WAN Qiang1, WANG Qun1, WANG Rong1. Emodin ameliorates high-glucose-induced mesangial cell hypocontractility[J]. JOURNAL OF SHANDONG UNIVERSITY (HEALTH SCIENCES), 2010, 48(9): 14-18.

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