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分离的线粒体和细胞质的代谢谱分析揭示了特定区室的代谢反应。

Metabolic profiling of isolated mitochondria and cytoplasm reveals compartment-specific metabolic responses.

作者信息

Pan Daqiang, Lindau Caroline, Lagies Simon, Wiedemann Nils, Kammerer Bernd

机构信息

Center for Biological Systems Analysis, ZBSA, Albert-Ludwigs-University Freiburg, Habsburgerstraße 49, 79104, Freiburg, Germany.

Institute of Pharmaceutical Sciences, Albert-Ludwigs-University Freiburg, 79104, Freiburg, Germany.

出版信息

Metabolomics. 2018;14(5):59. doi: 10.1007/s11306-018-1352-x. Epub 2018 Mar 31.

Abstract

INTRODUCTION

Subcellular compartmentalization enables eukaryotic cells to carry out different reactions at the same time, resulting in different metabolite pools in the subcellular compartments. Thus, mutations affecting the mitochondrial energy metabolism could cause different metabolic alterations in mitochondria compared to the cytoplasm. Given that the metabolite pool in the cytosol is larger than that of other subcellular compartments, metabolic profiling of total cells could miss these compartment-specific metabolic alterations.

OBJECTIVES

To reveal compartment-specific metabolic differences, mitochondria and the cytoplasmic fraction of baker's yeast were isolated and subjected to metabolic profiling.

METHODS

Mitochondria were isolated through differential centrifugation and were analyzed together with the remaining cytoplasm by gas chromatography-mass spectrometry (GC-MS) based metabolic profiling.

RESULTS

Seventy-two metabolites were identified, of which eight were found exclusively in mitochondria and sixteen exclusively in the cytoplasm. Based on the metabolic signature of mitochondria and of the cytoplasm, mutants of the succinate dehydrogenase (respiratory chain complex II) and of the FF-ATP-synthase (complex V) can be discriminated in both compartments by principal component analysis from wild-type and each other. These mitochondrial oxidative phosphorylation machinery mutants altered not only citric acid cycle related metabolites but also amino acids, fatty acids, purine and pyrimidine intermediates and others.

CONCLUSION

By applying metabolomics to isolated mitochondria and the corresponding cytoplasm, compartment-specific metabolic signatures can be identified. This subcellular metabolomics analysis is a powerful tool to study the molecular mechanism of compartment-specific metabolic homeostasis in response to mutations affecting the mitochondrial metabolism.

摘要

引言

亚细胞区室化使真核细胞能够同时进行不同的反应,导致亚细胞区室中存在不同的代谢物池。因此,与细胞质相比,影响线粒体能量代谢的突变可能会导致线粒体中不同的代谢改变。鉴于细胞质中的代谢物池比其他亚细胞区室的代谢物池大,全细胞的代谢谱分析可能会遗漏这些区室特异性的代谢改变。

目的

为了揭示区室特异性的代谢差异,分离了面包酵母的线粒体和细胞质部分,并对其进行代谢谱分析。

方法

通过差速离心分离线粒体,并与剩余的细胞质一起通过基于气相色谱-质谱(GC-MS)的代谢谱分析进行分析。

结果

共鉴定出72种代谢物,其中8种仅在线粒体中发现,16种仅在细胞质中发现。基于线粒体和细胞质的代谢特征,通过主成分分析,可以将琥珀酸脱氢酶(呼吸链复合物II)和FF-ATP合酶(复合物V)的突变体与野生型以及彼此区分开来。这些线粒体氧化磷酸化机制突变体不仅改变了柠檬酸循环相关的代谢物,还改变了氨基酸、脂肪酸、嘌呤和嘧啶中间体等。

结论

通过将代谢组学应用于分离的线粒体和相应的细胞质,可以鉴定区室特异性的代谢特征。这种亚细胞代谢组学分析是研究影响线粒体代谢的突变响应中区室特异性代谢稳态分子机制的有力工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dea1/5878833/33779868a676/11306_2018_1352_Fig1_HTML.jpg

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