期刊文献+
任意字段
题名或关键词
题名
关键词
文摘
作者
第一作者
机构
刊名
分类号
参考文献
作者简介
基金资助
栏目信息

实时分析UV诱导的细胞凋亡过程中Bax的转位

Real-time Analysis of Bax Translocation during UV-induced Apoptosis
在线阅读 下载PDF
导出
摘要 Bax(Bcl-2-associated X protein)是bcl-2家族中的一个很重要的促凋亡蛋白,在正常的细胞生理状态下,主要分布在细胞质,在UV等凋亡刺激因子的作用下,则从细胞质转位到线粒体从而诱导细胞色素C的释放,最终引起细胞凋亡。缺失Bax的细胞对UV诱导的细胞凋亡有抗性,因此研究Bax的特性有助于深入了解UV诱导的细胞凋亡信号转导通路的分子机制。以前的研究大都采用生化的手段,无法在活细胞上实时动态的观察Bax蛋白的变化过程。运用激光共聚焦扫描显微成像技术单细胞实时检测了UV诱导的细胞凋亡过程中Bax的动态变化过程。研究结果表明:UV诱导的细胞凋亡过程中Bax的转位大约起始于UV照射后5 h-6 h,整个转位过程持续20 min-30 min。 Bax, a proapoptotic member of the Bcl-2 family, localizes largely in the cytoplasm but redistributes to mitochondria and undergoes oligomerization to induce the release of apoptogenic factors such as cytochrome c in response to apoptotic stimuli. Cells deficient in Bax are resistant to UV-induced apoptosis. Thus, studying Bax translocation is very important for us to understand the cellular signaling mechanisms mediating UV-induced apoptosis. Most of previous studies on Bax translocation were done by western blotting or immunoblotting, but these techniques could not monitor the translocation of intracellular Bax in real time. In this study, we monitored the dynamics of Bax translocation during UV- induced apoptosis in single living cell using laser confocal microscope imaging technique. These results demonstrated that Bax translocation was initiated at 5 h - 6 h after UV irradiation, the average duration of this course was 20 min - 30min.
作者 吴银院 邢达 陈同生
机构地区 华南师范大学激光生命科学研究所暨激光生命科学教育部重点实验室
出处 《激光生物学报》 CAS CSCD 2007年第2期135-138,共4页 Acta Laser Biology Sinica
基金 国家自然科学基金面上项目(60378043 30470494) 广东省自然科学基金项目(015012 04010394) 广东省科技计划项目(2004B10401011)资助
关键词 BAX蛋白 细胞凋亡 UV Bax apoptosis UV
分类号 Q274 [生物学—细胞生物学]
  • 相关文献

参考文献12

  • 1KERR J F,WYLLIE A H,CURRIE A R.Apoptosis:a Basic Biological Phenomenon with Wild-ranging Implications in Tissue Kinetics[J].Br J Cancer,1972,26:239-257.
  • 2ADAMS J M,CORY S.The Bcl-2 Protein Family:Arbiters of Cell Survival[J].Science,1998,281:1322-1326.
  • 3陈同生,王进军,邢达,王方.细胞凋亡过程中Bid蛋白在活细胞内的动态分布[J].激光生物学报,2005,14(4):279-282. 被引量:9
  • 4WANG Jin-jun,CHEN Tong-sheng,XING Da,et al.Observation of Interaction between Bid and 14-3-3 Proteins by FRET in Living Cell during TNF-a-induced Apoptosis[ C ].Proc SPIE,2004,5630:608-616.
  • 5MAURER M,TSAI M,METZ M.et al.A Role for Bax in the Regulation of Apoptosis in Mouse Mast Cells[ J].J Invest Dermatol,2000,114(6):1205-1206.
  • 6WEI M C,LINDSTEN T,MOOTHA V K.tBID,a Membranetargeted Death Ligand,Oligomerizes Bak to Release Cytochrome C[J].Genes Der,2000,14:2060-2071.
  • 7CHIPUK J,KUWANA T,BOUCHIER-HAYES L,et al.Direct Activation of Bax by p53 Mediates Mitochondrial Membrane Permeabilization and Apoptosis[ J ].Science,2004,303:1010-1014.
  • 8TSURUT A F,MASUYAMA N,GOTOH Y.The Phosphatidylinositol 3-Kinase (PI3K) akt Pathway Suppresses Bax Translocation to Mitochondria[ J].J Biol Chem,2002,277 (16):14040-14047.
  • 9NECHUSHTAN A,SMITH C L,HSU Y T,et al.Conformation of the Bax C-terminus Regulates Subcellular Location and Cell Death[ J].EMBO J,1999,8:2330-2341.
  • 10ESKES R,ANTONSSON B,OSEN-SAND A,et al.Bax-induced Cytochrome C Release from Mitochondria is Independent of the Permeability Transition Pore but Highly Dependent on Mg2+ Ions[J].J Cell Biol,1998,143:217-224.

二级参考文献9

  • 1WANG K, YIN X M, CHAO D T, MILLIMAN C L, et al.BID: A Novel BH3 domain-only death agonist[J]. Genes Develop, 1996, 10 (22): 2859-2869.
  • 2KORSMEYER S J, WEI M C, SAITO M, et al. Pro-apoptotic cascade activates BID, which oligomerizes BAK or BAX into pores that result in the release of cytochrome c[J]. Cell Death Diff, 2000, 7 (12): 1166-1173.
  • 3KIM T H, ZHAO Y, BARBER M J, et al. Bid-induced cytochrome c release is mediated by a pathway independent of mitochondrial permeability transition pore and Bax[J]. J Biol Chem, 2000, 275 (50): 39474-39481.
  • 4YIN X M, WANG K, GROSS A, et al. Bid-deficient mice are resistant to Fas-induced hepatocellular apoptosis[J]. Nature, 1999, 400 (6747): 886-891.
  • 5WEI M C, LINDSEN T, MOOTHA V K, et al. tBID, a membrane-targeted death ligand, oligomerizes BAK to release cytochrome c[J]. Genes Dev, 2000, 14 (16): 2060-2071.
  • 6LI H, ZHU H, XU C, et al. Cleavage of BID by caspase8mediates the mitochondrial damage in the Fas pathway of apoptosis[J]. Cell, 1998, 94 (4): 491-501.
  • 7GROSS A, YIN X M, WANG K, et al. Caspase cleaved BID targets mitochondria and is required for cytochrome c release,while BCL-XL prevents this release but not tunor necrosis factor-R1/Fas death[J]. J Biol Chem, 1999, 274 (2):1156-1163.
  • 8LUO X, BUDIHARDJO I, ZOU H, et al. Bid, a Bcl2 interacting protein, mediates cytochrome c release fiom mitochondria in response to activation of cell surface death receptors [J]. Cell, 1998, 94 (4): 481-490.
  • 9ZHA J, WEILER S, OHK J, et al. Posttranslational N-myristoylation of BID as a molecular switch for targeting mitochondria and apoptosis [ J ]. Science, 2000, 290 (5497):1761-1765.

共引文献8

激光生物学报
2007年 第2期

相关作者

内容加载中请稍等...

相关机构

内容加载中请稍等...

相关主题

内容加载中请稍等...

浏览历史

内容加载中请稍等...
;
使用帮助 返回顶部