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Transformations of the macromolecular landscape at mitochondria during DNA-damage-induced apoptotic cell death

机译:DNA损伤诱导的凋亡细胞死亡过程中线粒体大分子景观的转变

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Apoptosis is a dynamic process regulated by mitochondrion critical for cellular respiration and survival. Execution of apoptosis is mediated by multiple protein signaling events at mitochondria. Initiation and progression of apoptosis require numerous apoptogenic factors that are either released from or sequestered in mitochondria, which may transform the biomolecular makeup of the organelle. In this communication, using Raman microspectroscopy, we demonstrate that transformation in biomolecular composition of mitochondrion may be used as apoptosis marker in an individual cell. For the first time, we show that significant changes occur in the concentrations of RNA, DNA, protein, and lipid constituents of mitochondria during apoptosis. The structural analysis of proteins on mitochondria demonstrated a decrease in α -helix secondary structure content, and an increase in the levels of random coils and β -sheets on mitochondria. This may represent an additional hallmark of apoptosis. Strikingly, we observed nearly identical changes in macromolecular content of mitochondria both in the presence and absence of a key proapoptotic protein, Bax (Bcl-2-associated X protein). Increased DNA level in mitochondria corresponded with higher mitochondrial DNA (mtDNA), cellular reactive oxygen species (ROS), and mitochondrial ROS production. Upregulation of polymerase- γ (POLG), mitochondrial helicase Twinkle, and mitochondrial transcription factor A (Tfam) in response to DNA damage correlated with increased mtDNA and RNA synthesis. Elevated activity of oxidative phosphorylation complexes supports functional mitochondrial respiration during apoptosis. Thus, we define previously unknown dynamic correlation of macromolecular structure of mitochondria and apoptosis progression in the presence and absence of Bax protein. These findings open up a new approach for monitoring physiological status of cells by non invasive single-cell method. Cell Death and Disease (2014) 5, e1453; doi: 10.1038/cddis.2014.405 ; published online 9 October 2014
机译:凋亡是由线粒体调节的动态过程,对细胞呼吸和存活至关重要。凋亡的执行是由线粒体中的多种蛋白质信号传递事件介导的。凋亡的开始和进展需要从线粒体中释放或隔离在线粒体中的众多凋亡原性因子,这可能会改变细胞器的生物分子组成。在此交流中,使用拉曼光谱,我们证明了线粒体生物分子组成中的转化可用作单个细胞中的凋亡标记。第一次,我们显示凋亡过程中线粒体的RNA,DNA,蛋白质和脂质成分的浓度发生了显着变化。线粒体上蛋白质的结构分析表明,线粒体上α-螺旋二级结构含量降低,无规卷曲和β-折叠水平增加。这可能代表了凋亡的另一个标志。令人惊讶的是,我们观察到,无论是否存在关键的促凋亡蛋白Bax(Bcl-2相关X蛋白),线粒体大分子含量的变化几乎相同。线粒体中DNA含量的增加与线粒体DNA(mtDNA),细胞活性氧(ROS)和线粒体ROS生成量较高相对应。响应DNA损伤,聚合酶γ(POLG),线粒体解旋酶Twinkle和线粒体转录因子A(Tfam)上调与mtDNA和RNA合成增加有关。氧化磷酸化复合物的活性升高支持凋亡过程中的线粒体呼吸功能。因此,我们定义了先前未知的线粒体大分子结构与存在和不存在Bax蛋白的细胞凋亡进程之间的动态相关性。这些发现为通过无创单细胞方法监测细胞的生理状态开辟了新途径。 Cell Death and Disease(2014)5,e1453; doi:10.1038 / cddis.2014.405; 2014年10月9日在线发布

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