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Mitochondrial protein functions elucidated by multi-omic mass spectrometry profiling

机译:多功能质谱分析法阐明线粒体蛋白功能

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Mitochondrial dysfunction is associated with many human diseases, including cancer and neurodegeneration, that are often linked to proteins and pathways that are not well-characterized. To begin defining the functions of such poorly characterized proteins, we used mass spectrometry to map the proteomes, lipidomes, and metabolomes of 174 yeast strains, each lacking a single gene related to mitochondrial biology. 144 of these genes have human homologs, 60 of which are associated with disease and 39 of which are uncharacterized. We present a multi-omic data analysis and visualization tool that we use to find covariance networks that can predict molecular functions, correlations between profiles of related gene deletions, gene-specific perturbations that reflect protein functions, and a global respiration deficiency response. Using this multi-omic approach, we link seven proteins including Hfd1p and its human homolog ALDH3A1 to mitochondrial coenzyme Q (CoQ) biosynthesis, an essential pathway disrupted in many human diseases. This Resource should provide molecular insights into mitochondrial protein functions.
机译:线粒体功能障碍与许多人类疾病(包括癌症和神经退行性疾病)相关,这些疾病通常与蛋白质和尚未明确表征的途径有关。为了开始定义此类特征较差的蛋白质的功能,我们使用质谱法绘制了174个酵母菌株的蛋白质组,脂质组和代谢组的图谱,每个菌株都缺少与线粒体生物学相关的单个基因。这些基因中的144个具有人类同源物,其中60个与疾病有关,而39个未鉴定。我们提供了一种多组数据分析和可视化工具,用于查找可以预测分子功能的协方差网络,相关基因缺失的概况之间的相关性,反映蛋白质功能的特定基因扰动以及全球呼吸不足反应。使用这种多组学方法,我们将包括Hfd1p及其人类同源物ALDH3A1在内的7种蛋白与线粒体辅酶Q(CoQ)生物合成连接,这是在许多人类疾病中都被破坏的重要途径。该资源应提供线粒体蛋白质功能的分子见解。

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