奥氮平对骨髓间充质干细胞成脂分化的作用及机制

doi:10.16098/j.issn.0529-1356.2016.03.009

解剖学报 ›› 2016, Vol. ›› Issue (3): 341-347.doi: 10.16098/j.issn.0529-1356.2016.03.009

奥氮平对骨髓间充质干细胞成脂分化的作用及机制

纪晨燕^1,2李永海^1,2* 李萌^1,2杨海杰^1,2冯志伟^2

1. 新乡医学院生命科学技术学院，河南新乡 453003; 2.河南省干细胞与生物治疗工程研究中心，河南新乡 453003

收稿日期:2015-12-02 修回日期:2016-01-25 出版日期:2016-06-06 发布日期:2016-06-06
通讯作者: 李永海 E-mail:yonghaili@126.com
基金资助:
河南省科技厅省院合作项目;新乡医学院校内培育基金;新乡医学院研究生科研创新支持计划资助项目

Effects and mechanism of olanzapine on the adipose differentiation of mouse bone marrow mesenchymal stem cells

JI Chen-yan ^1,2LI Yong-hai ^1,2*LI Meng ^1,2YANG Hai-jie^1,2 FENG Zhi-wei²

1.Collage of Life Science and Technology，Xinxiang Medical University, He’nan Xinxiang 453003, China; 2.Stem Cell and Biotherapy Engineering Research Center of Henan Province, He’nan Xinxiang 453003, China

Received:2015-12-02 Revised:2016-01-25 Online:2016-06-06 Published:2016-06-06
Contact: LI Yong-hai E-mail:yonghaili@126.com
Supported by:
Supported by Cooperation project of Chinese Academy of Sciences of Henan Province;Intramural science fostering foundation of Xinxiang Medical University;Graduate student research and innovation project

摘要/Abstract

摘要：

目的探讨第2代抗精神病药物(SGA)奥氮平(olanzapine)对小鼠骨髓间充质干细胞（BMSCs）体外脂肪分化的影响及其作用机制。方法培养小鼠BMSCs，MTT法检测不同浓度奥氮平对BMSCs增殖的影响；通过油红O染色观察细胞形态，Western blotting检测脂肪分化标志基因蛋白αP2和C/EBPβ的表达， Real-time PCR检测成脂相关基因Leptin、C/EBPα和TNF-α的mRNA表达情况；同时Western blotting检测Akt信号通路上下游相关分子的表达水平及磷脂酰肌醇3激酶（PI3K）/Akt特异性阻断剂对小鼠BMSCs脂肪分化的影响。结果 MTT法结果显示，20μmol/L奥氮平对BMSCs的毒性最小；油红O染色可见加入奥氮平的细胞内脂肪滴明显多于对照组；Western blotting结果显示，αP2和C/EBPβ的表达水平较对照组上升了36%(P<0.01)和25%(P<0.05);Real-time PCR结果显示,Leptin、C/EBPα和TNF-α的表达水平较对照组分别上升68%（P<0.001）、79%（P<0.01）和60%（P<0.01），均具有统计学意义；Western blotting检测结果显示，p-Akt的含量明显高于对照组，磷酸化糖原合成激酶3β（p-GSK-3β）的表达随着p-Akt表达的增加逐渐减少；加入PI3K/Akt特异性阻断剂(LY294002)后αP2和C/EBPβ的表达受到抑制，细胞中的脂肪滴也明显减少。结论奥氮平可能通过促使PI3K/Akt信号通路中Akt的磷酸化水平升高来促进小鼠BMSCs的脂肪分化。

Abstract:

Objective To investigate the effects of olanzapine on the adipose differentiation and mechanism of mouse bone marrow mesenchymal stem cells(BMSCs).
Methods MTT colorimetry was used for assaying different concentrations of olanzapine on the proliferation of mouse BMSCs. The morphology of cells was observed by Oil red O staining. The expressions levels of adipocyte markers αP2 and C/EBPβ were detected by Western blotting, mRNA expression levels of the related genes of Leptin, C/EBPα and TNF-α were analyzed by Real-time PCR. The protein expression of Akt signaling pathway related molecules and effects of phosphatidylinositol 3 kinase (PI3K)/Akt inhibitor on the differentiation of BMSCs were determined by Western blotting. Results The results of MTT colorimetry showed that 20μmol/L olanzapine had minimal toxicity on BMSCs. Oil red O staining showed that intracellular lipid droplets in the experimental group were significantly more than the control group. The results of Western blotting showed that the expression levels of αP2 and C/EBPβ increased by about 36%(P<0.01) and 25%(P<0.05) compared with the control group respectively. The results of Real-time PCR showed that the expression levels of adipogenic genes Leptin, C/EBPα and TNF-α significantly increased than the control group, increased about 68%（P<0.001）,79%（P<0.01）and 60%（P<0.01）respectively. The expression levels of p-Akt were significantly higher than the control group, the expression of glycogen synthase kinase 3β(GSK-3β) with the increase of p-Akt expression gradually reduced. The expression levels of αP2 and C/EBPβ were inhibited after BMSCs were pretreated with PI3K/Akt inhibitor (LY294002). Oil red O staining results showed fat droplets in cells also decreased significantly. Conclusion Olanzapine may elevate the expression level of p-Akt of PI3K/AKT signaling pathway to promote the adipogenic differentiation of mouse BMSCs.

纪晨燕李永海* 李萌杨海杰冯志伟. 奥氮平对骨髓间充质干细胞成脂分化的作用及机制[J]. 解剖学报, 2016, (3): 341-347.

JI Chen-yanLI Yong-hai*LI MengYANG Hai-jie FENG Zhi-wei . Effects and mechanism of olanzapine on the adipose differentiation of mouse bone marrow mesenchymal stem cells[J]. AAS, 2016, (3): 341-347.

参考文献

［1］Wang YL,He XM,Tang W,et al.Effect of stromal cell derived factor-1α/CXCR4/CXCR7 axis on migration of the bone marrow mesenchymal stem cells.［J］.Acta Anatomica Sinica,2014,45(5): 639-645.(in Chinese) 
王玉兰，何晓梅，唐薇，等.基质细胞衍生因子-1α/CXCR4/CXCR7轴对骨髓间充质干细胞迁移的影响［J］.解剖学报，2014，45（5）：639-645.
［2］Altiok S, Xu M, Spiegelman BM. PPARgamma induces cell cycle withdrawal:inhibition of E2F/DP DNA-binding activity via downregulation of PP2A［J］.Genes Dev, 1997, 11(15): 1987-1988.
［3］Lin FT, Lane MD. CCAAT/enhancer binding protein alpha is sufficient to initiate the 3T3-L1 adipocyte differentiation program ［J］. Proc Natl Acad Sci USA, 1994, 91(19): 8757-8761.
［4］Bridler R, Umbricht D. Atypical antipsychotics in the treatment of schizophrenia［J］. Swiss Med Wkly, 2003, 133(5-6):63-76
［5］Keefe RS, Young CA, Rock SL, et al. One-year double-blind study of the neurocognitive efficacy of olanzapine, risperidone,and haloperidol in schizophrenia［J］. Schizophr Res, 2006, 81(1):1-15.
［6］McDougle CJ, Stigler KA, Erickson CA, et al. Atypical antipsychotics in children andadolescents with autistic and other pervasive developmental disorders［J］. Clin Psychiatry, 2008, 69(4):15-20.
［7］Papakostas GI, Shelton RC. Use of atypical antipsychotics for treatment-resistant major depressive disorder［J］. Curr Psychiatry Rep, 2008, 10(6):481-486.
［8］Pfeifer JC, Kowatch RA, DelBello MP. Pharmacotherapy of bipolar disorder in children and adolescents: recent progress［J］. CNS Drugs, 2010, 24(7):575-593.
［9］Newcomer JW. Metabolic considerations in the use of antipsychotic medications: a review of recent evidence［J］. J Clin Psychiatry, 2007(68): 20-27.
［10］Panagiotopoulos C, Ronsley R, Davidson J. Increased prevalence of obesity and glucose intolerance in youth treated with second-generation antipsychotic medications［J］.Can J Psychiatry, 2009, 54(11): 743-749.
［11］Tong Q, Hotamisligil GS. Molecular mechanisms of adipocyte differentiation［J］.Rev Endocr Metab Disord,2001, 2(4): 349-355.
［12］Camp HS, Ren D, Left T. Adipogenesis and fat-cell function in obesity and diabetes［J］.Trends Mol Meal, 2002, 8(9):442-447.
［13］Minet-Ringuet J, Even PC, Valet P, et al. Alterations of lipid metabolism and gene expression in rat adipocytes during chronic olanzapine treatment［J］. Mol Psychiatry, 2007, 12(6): 562-571.
［14］Vestri HS, Maianu L, Moellering DR, et al. Atypical antipsychotic drugs directly impair insulin action in adipocytes: effects on glucose transport, lipogenesis, and antilipolysis［J］. Neuropsychopharmacology, 2006, 32(4):765-772.
［15］Yang LH, Chen TM, Yu ST, et al. Olanzapine induces SREBP-1-related adipogenesis in 3T3-L1 cells［J］. Pharmacol Res, 2007, 56(3): 202-208.
［16］Yang Z, Yin JY, Gong ZC, et al. Evidence for an effect of clozapine on the regulation of fat-cell derived factors［J］. Clin Chim Acta 2009, 408(1-2): 98-104.
［17］Shi Y, Xia YY, Wang L, et al. Neural cell adhesion molecule modulates mesenchymal stromal cell migration via activation of MAPK/ERK signaling［J］.Exp CellRes, 2012, 318(17):2257-2267.
［18］Spalding KL, Arner E, Westermark PO, et al. Dynamics of fat cell turnover in humans［J］. Nature, 2008, 453(7196):783-787.
［19］Sertié AL, Suzuki AM, Sertié RA. Effects of antipsychotics with different weight gain liabilities on human in vitro models of adipose tissue differentiation and metabolism［J］. Prog Neuropsychopharmacol Biol Psychiatry, 2011,35(8):1884-1890.
［20］Vestri HS, Maianu L, Moellering DR, et al. Atypical antipsychotic drugs directly impair insulin action in adipocytes: effects on glucose transport, lipogenesis, and antilipolysis［J］.Neuropsychopharmacology, 2006, 32(4):765-772.
［21］Brazil DP, Yang ZZ, Hemmings BA. Advances in protein kinase B signalling: AKTion on multiple fronts［J］. Trends Biochem Sci, 2004, 29(5): 233-242.
［22］Panariello F, Perruolo G, Cassese A. Clozapine impairs insulin action by up-regulating Akt phosphorylation and Ped/Pea-15 protein abundance［J］. J Cell Physiol, 2012, 227(4):1485-1492.
［23］Gu D, Yu B, Zhao C, et al. The effect of pleiotrophin signaling on adipogenesis ［J］. FEBS Lett, 2007, 581(3):382-388.
［24］Yang HJ, Xia YY, Wang L, et al. A novel role for neural cell adhesion molecule in modulating insulin signaling and adipocyte differentiation of mouse mesenchymal stem cells ［J］. J Cell Sci, 2011, 124(Pt 15): 2552-2560.

奥氮平对骨髓间充质干细胞成脂分化的作用及机制

Effects and mechanism of olanzapine on the adipose differentiation of mouse bone marrow mesenchymal stem cells

可视化

摘要/Abstract

引用本文

使用本文

参考文献

相关文章 0

编辑推荐

Metrics

本文评价