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《心脏杂志》[ISSN:1009-7236/CN:61-1268/R]

期数:

2009年第2期

页码:

169

栏目:

基础研究

出版日期:

2009-03-30

文章信息/Info

Title:

Relationship between Bcl-2/Bax and staurosporine-induced rat cardiomyocyte apoptosis

作者:

刘安恒¹; ³; 张卫卫¹; 曹亚南¹; 师堂旺¹; 刘艳¹; 张金平²; 王晓明¹

第四军医大学西京医院:1.老年病科,2.中医研究所，陕西 西安 710032; 3.军事医学科学院附属307医院心内科，北京，100071

Author(s):

LIU An-heng¹; ³;  ZHANG Wei-wei¹;  CAO Ya-nan¹;  SHI Tang-wang¹;  LIU Yan¹;  ZHANG Jin-ping²;  WANG Xiao-ming¹

1.Department of Geriatrics, 2.Institute of Chinese Medicine, Xijing Hospital, Fourth Military Medical University, Xi’an 710032, Shaanxi, China; 3.Department of Cardiology, PLA 307 Hospital, Academy of Military Medical Sciences, Beijing, 100071, China;

关键词:

心肌细胞; 凋亡; staurosporine; Bcl-2/Bax

Keywords:

cardiomyocyte;  apoptosis;  staurosporine;  Bcl-2/Bax

分类号:

R329.2

DOI:

-

文献标识码:

A

摘要:

目的 探讨staurosporine（STS）诱导心肌细胞凋亡过程中，凋亡调节蛋白Bcl-2和Bax的变化及意义。方法 以STS诱导原代培养的SD乳鼠心肌细胞，检测半胱天冬蛋白酶(caspase)-3的活性及用Hoechst-33258荧光染色观察细胞凋亡。用免疫印迹法（Western blot）检测Bcl-2和Bax表达的变化。用免疫荧光共聚焦显微镜和免疫印迹法观察Bax在细胞内的分布。结果 以4 μmol/L STS处理心肌细胞，随着处理时间的延长，细胞中caspase-3的活性逐渐增加，与对照组比较，8 h达到峰值（P<0.01）。Hoechst-33258荧光染色显示，多数细胞核呈现核分叶。STS诱导心肌细胞凋亡过程中，Bcl-2和Bax的水平与对照组比较无显著变化。正常细胞内的Bax均匀分布于细胞质中，在STS处理的细胞中，Bax明显聚集于线粒体上，呈现明显的线粒体的转位。STS诱导心肌细胞凋亡过程中，胞质片段Bax的水平明显下降，而线粒体片段Bax的水平明显升高，进一步证实STS诱导细胞凋亡过程中伴有明显的Bax线粒体转位。结论 STS诱导细胞凋亡中，伴有明显的Bax由胞质向线粒体的转位。

Abstract:

AIM To explore the changes of Bcl-2/Bax and significance in staurosporine（STS）induced cardiomyocyte apoptosis. METHODS Primary cultured neonatal rat cardiomyocytes were exposed to STS to induce apoptosis. Cell apoptosis was determined by cysteine aspartate specific proteinase(caspase)-3 activity and Hoechst 33258 staining. Bcl-2/Bax expression was measured by Western blot and Bax translocation was assessed by double immunofluorescence labeling as well as Western blot. RESULTS Exposure of cardiomyocytes to STS (4 μmol/L) resulted in an increase of caspase-3 activity in a time-dependent manner with a peak at 8 h. Hoechst 33258 fluorescence staining showed many segmented and irregularly shaped nuclei and STS induction did not alter Bcl-2/Bax levels. In normal cardiomyocytes, a diffuse localization of Bax was primarily found in the cytoplasm. In contrast, exposure of cells to STS resulted in Bax translocation from cytoplasm to mitochondria. Western blot also demonstrated that an increase in mitochondrial Bax level was accompanied by a concomitant decrease in cytosolic Bax level, which provided some direct evidence that a significant increased Bax translocation existed in the STS-induced cell apoptosis. CONCLUSION STS induces a significant pro-apoptotic Bax translocation to mitochondria in cardiomyocyte apoptosis, a mechanism that may be involved in STS-induced cell apoptosis.

参考文献/References

[1］ Haunstetter A, Izumo S. Future perspectives and potential implications of cardiac myocyte apoptosis［J］. Cardiovasc Res, 2000, 45(3):795-801.

［2］ Gustafsson AB, Gottlieb RA. Bcl-2 family members and apoptosis, taken to heart［J］. Am J Physiol Cell Physiol, 2007, 292(1):C45-C51.

［3］ Kang PM, Izumo S. Apoptosis in heart: basic mechanisms and implications in cardiovascular diseases［J］. Trends Mol Med, 2003,9(4):177-182.

［4］ O’Rourke B. Apoptosis: rekindling the mitochondrial fire［J］. Circ Res, 1999, 85(10):880-883.

［5］ Tanabe S, Wang X, Takahashi N, et al. HCO-3-independent rescue from apoptosis by stilbene derivatives in rat cardiomyocytes［J］. FEBS Lett, 2005, 579(2):517-522.

［6］ Barth E, Stammler G, Speiser B, et al. Ultrastructural quantitation of mitochondria and myofilaments in cardiac muscle from 10 different animal species including man［J］. J Mol Cell Cardiol,1992, 24(7):669-681.

［7］ Haunstetter A, Izumo S. Apoptosis: basic mechanisms and implications for cardiovascular disease［J］. Circ Res, 1998, 82(11):1111-1129.

［8］ Condorelli G, Morisco C, Stassi G, et al. Increased cardiomyocyte apoptosis and changes in proapoptotic and antiapoptotic genes bax and bcl-2 during left ventricular adaptations to chronic pressure overload in the rat［J］. Circulation, 1999, 99(23):3071-3078.

［9］ Iida KT, Suzuki H, Sone H, et al. Insulin inhibits apoptosis of macrophage cell line, THP-1 cells, via phosphatidylinositol-3-kinase-dependent pathway［J］. Arterioscler Thromb Vasc Biol, 2002, 22(3):380-386.

［10］Kutuk O, Basaga H. Bcl-2 protein family: implications in vascular apoptosis and atherosclerosis［J］. Apoptosis, 2006, 11(10):1661-1675.

［11］Kukreja RC, Xi L. eNOS phosphorylation: a pivotal molecular switch in vasodilation and cardioprotection?［J］. J Mol Cell Cardiol, 2007, 42(2):280-282.

［12］Bajt ML, Farhood A, Lemasters JJ, et al. Mitochondrial bax translocation accelerates DNA fragmentation and cell necrosis in a murine model of acetaminophen hepatotoxicity［J］. J Pharmacol Exp Ther, 2007, 324(1):8-14.

［13］Tikhomirov O, Carpenter G. Bax activation and translocation to mitochondria mediate EGF-induced programmed cell death［J］. J Cell Sci, 2005, 118(Pt 24):5681-5690.

备注/Memo

备注/Memo:

收稿日期：2008-6-19.基金项目：国家自然基金课题项目资助（30570758，30770847） 通讯作者：王晓明，副教授，博士，主要从事心血管疾病的基础与临床研究Email:xmwang@fmmu.edu.cn 作者简介：刘安恒，主治医师，博士Email:doctorlah@126.com

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更新日期/Last Update: 2009-04-16