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化脓性链球菌与人类血浆蛋白相互作用网络的综合分析。

A comprehensive analysis of the Streptococcus pyogenes and human plasma protein interaction network.

作者信息

Sjöholm Kristoffer, Karlsson Christofer, Linder Adam, Malmström Johan

机构信息

Department of Immunotechnology, Faculty of Engineering, Lund University, Sweden.

出版信息

Mol Biosyst. 2014 Jul;10(7):1698-708. doi: 10.1039/c3mb70555b. Epub 2014 Feb 14.

Abstract

Streptococcus pyogenes is a major human bacterial pathogen responsible for severe and invasive disease associated with high mortality rates. The bacterium interacts with several human blood plasma proteins and clarifying these interactions and their biological consequences will help to explain the progression from mild to severe infections. In this study, we used a combination of mass spectrometry (MS) based techniques to comprehensively quantify the components of the S. pyogenes-plasma protein interaction network. From an initial list of 181 interacting human plasma proteins defined using liquid chromatography (LC)-MS/MS analysis we further subdivided the interacting protein list using selected reaction monitoring (SRM) depending on the level of enrichment and protein concentration on the bacterial surface. The combination of MS methods revealed several previously characterized interactions between the S. pyogenes surface and human plasma along with many more, so far uncharacterised, possible plasma protein interactions with S. pyogenes. In follow-up experiments, the combination of MS techniques was applied to study differences in protein binding to a S. pyogenes wild type strain and an isogenic mutant lacking several important virulence factors, and a unique pair of invasive and non-invasive S. pyogenes isolates from the same patient. Comparing the plasma protein-binding properties of the wild type and the mutant and the invasive and non-invasive S. pyogenes bacteria revealed considerable differences, underlining the significance of these protein interactions. The results also demonstrate the power of the developed mass spectrometry method to investigate host-microbial relationships with a large proteomics depth and high quantitative accuracy.

摘要

化脓性链球菌是一种主要的人类细菌病原体,可引发严重且具有侵袭性的疾病,死亡率很高。该细菌与多种人类血浆蛋白相互作用,阐明这些相互作用及其生物学后果将有助于解释从轻度感染到重度感染的进展过程。在本研究中,我们结合使用了基于质谱(MS)的技术,以全面定量化脓性链球菌 - 血浆蛋白相互作用网络的组成成分。从使用液相色谱(LC)-MS/MS分析确定的181种相互作用的人类血浆蛋白的初始列表中,我们根据细菌表面的富集水平和蛋白质浓度,使用选择反应监测(SRM)进一步细分了相互作用蛋白列表。质谱方法的结合揭示了化脓性链球菌表面与人类血浆之间几种先前已表征的相互作用,以及更多迄今为止未表征的、可能的化脓性链球菌与血浆蛋白的相互作用。在后续实验中,质谱技术的组合被用于研究蛋白质与化脓性链球菌野生型菌株以及缺乏几种重要毒力因子的同基因突变体,以及来自同一患者的一对独特的侵袭性和非侵袭性化脓性链球菌分离株结合的差异。比较野生型和突变体以及侵袭性和非侵袭性化脓性链球菌细菌的血浆蛋白结合特性,发现了相当大的差异,突出了这些蛋白质相互作用的重要性。结果还证明了所开发的质谱方法在以大蛋白质组学深度和高定量准确性研究宿主 - 微生物关系方面的强大功能。

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