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对人类成纤维细胞进行线粒体蛋白质组学研究以鉴定代谢失衡和细胞应激。

Mitochondrial proteomics on human fibroblasts for identification of metabolic imbalance and cellular stress.

作者信息

Palmfeldt Johan, Vang Søren, Stenbroen Vibeke, Pedersen Christina B, Christensen Jane H, Bross Peter, Gregersen Niels

机构信息

Institute of Clinical Medicine, Aarhus University Hospital, University of Aarhus, Denmark.

出版信息

Proteome Sci. 2009 May 28;7:20. doi: 10.1186/1477-5956-7-20.

Abstract

BACKGROUND

Mitochondrial proteins are central to various metabolic activities and are key regulators of apoptosis. Disturbance of mitochondrial proteins is therefore often associated with disease. Large scale protein data are required to capture the mitochondrial protein levels and mass spectrometry based proteomics is suitable for generating such data. To study the relative quantities of mitochondrial proteins in cells from cultivated human skin fibroblasts we applied a proteomic method based on nanoLC-MS/MS analysis of iTRAQ-labeled peptides.

RESULTS

When fibroblast cultures were exposed to mild metabolic stress - by cultivation in galactose medium- the amount of mitochondria appeared to be maintained whereas the levels of individual proteins were altered. Proteins of respiratory chain complex I and IV were increased together with NAD+-dependent isocitrate dehydrogenase of the citric acid cycle illustrating cellular strategies to cope with altered energy metabolism. Furthermore, quantitative protein data, with a median standard error below 6%, were obtained for the following mitochondrial pathways: fatty acid oxidation, citric acid cycle, respiratory chain, antioxidant systems, amino acid metabolism, mitochondrial translation, protein quality control, mitochondrial morphology and apoptosis.

CONCLUSION

The robust analytical platform in combination with a well-defined compendium of mitochondrial proteins allowed quantification of single proteins as well as mapping of entire pathways. This enabled characterization of the interplay between metabolism and stress response in human cells exposed to mild stress.

摘要

背景

线粒体蛋白是各种代谢活动的核心,是细胞凋亡的关键调节因子。因此,线粒体蛋白的紊乱常与疾病相关。需要大规模蛋白质数据来获取线粒体蛋白水平,基于质谱的蛋白质组学适用于生成此类数据。为了研究培养的人皮肤成纤维细胞中线粒体蛋白的相对含量,我们应用了一种基于对iTRAQ标记肽进行纳升液相色谱-串联质谱分析的蛋白质组学方法。

结果

当成纤维细胞培养物在半乳糖培养基中培养,暴露于轻度代谢应激时,线粒体数量似乎保持不变,而个别蛋白质的水平发生了改变。呼吸链复合体I和IV的蛋白质以及柠檬酸循环中依赖NAD+的异柠檬酸脱氢酶增加,这说明了细胞应对能量代谢改变的策略。此外,还获得了以下线粒体途径的定量蛋白质数据,中位标准误差低于6%:脂肪酸氧化、柠檬酸循环、呼吸链、抗氧化系统、氨基酸代谢、线粒体翻译、蛋白质质量控制、线粒体形态和细胞凋亡。

结论

强大的分析平台与明确的线粒体蛋白质汇编相结合,能够对单个蛋白质进行定量,并绘制整个途径的图谱。这使得我们能够表征暴露于轻度应激的人类细胞中代谢与应激反应之间的相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/31f0/2695441/bca14e784ffa/1477-5956-7-20-1.jpg

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