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大肠杆菌包膜蛋白质组及膜蛋白质组分析中的技术挑战

Proteome of the Escherichia coli envelope and technological challenges in membrane proteome analysis.

作者信息

Weiner Joel H, Li Liang

机构信息

Membrane Protein Research Group and The Institute for Biomolecular Design, University of Alberta, Canada.

出版信息

Biochim Biophys Acta. 2008 Sep;1778(9):1698-713. doi: 10.1016/j.bbamem.2007.07.020. Epub 2007 Aug 11.

Abstract

The envelope of Escherichia coli is a complex organelle composed of the outer membrane, periplasm-peptidoglycan layer and cytoplasmic membrane. Each compartment has a unique complement of proteins, the proteome. Determining the proteome of the envelope is essential for developing an in silico bacterial model, for determining cellular responses to environmental alterations, for determining the function of proteins encoded by genes of unknown function and for development and testing of new experimental technologies such as mass spectrometric methods for identifying and quantifying hydrophobic proteins. The availability of complete genomic information has led several groups to develop computer algorithms to predict the proteome of each part of the envelope by searching the genome for leader sequences, beta-sheet motifs and stretches of alpha-helical hydrophobic amino acids. In addition, published experimental data has been mined directly and by machine learning approaches. In this review we examine the somewhat confusing available literature and relate published experimental data to the most recent gene annotation of E. coli to describe the predicted and experimental proteome of each compartment. The problem of characterizing integral versus membrane-associated proteins is discussed. The E. coli envelope proteome provides an excellent test bed for developing mass spectrometric techniques for identifying hydrophobic proteins that have generally been refractory to analysis. We describe the gel based and solution based proteome analysis approaches along with protein cleavage and proteolysis methods that investigators are taking to tackle this difficult problem.

摘要

大肠杆菌的包膜是一种复杂的细胞器,由外膜、周质-肽聚糖层和细胞质膜组成。每个区室都有独特的蛋白质组合,即蛋白质组。确定包膜的蛋白质组对于开发计算机模拟细菌模型、确定细胞对环境变化的反应、确定功能未知基因所编码蛋白质的功能以及开发和测试新的实验技术(如用于鉴定和定量疏水蛋白质的质谱方法)至关重要。完整基因组信息的可得性促使多个研究小组开发计算机算法,通过在基因组中搜索前导序列、β-折叠基序和α-螺旋疏水氨基酸片段来预测包膜各部分的蛋白质组。此外,已发表的实验数据已通过直接挖掘和机器学习方法进行分析。在本综述中,我们审视了现有文献中有些令人困惑的内容,并将已发表的实验数据与大肠杆菌的最新基因注释相关联,以描述每个区室的预测蛋白质组和实验蛋白质组。文中讨论了区分整合蛋白与膜相关蛋白的问题。大肠杆菌包膜蛋白质组为开发用于鉴定通常难以分析的疏水蛋白质的质谱技术提供了一个绝佳的试验平台。我们描述了基于凝胶和基于溶液的蛋白质组分析方法,以及研究人员为解决这一难题所采用的蛋白质切割和蛋白水解方法。

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