蛋白质组
化学
猎枪
鸟枪蛋白质组学
微生物群
丰度(生态学)
基因组
计算生物学
生物化学
蛋白质组学
基因
生物信息学
生物
生态学
作者
Haonan Duan,Kai Cheng,Zhibin Ning,Leyuan Li,Janice Mayne,Zhuo Sun,Daniel Figeys
标识
DOI:10.1021/acs.analchem.2c02452
摘要
The human gut microbiome is a complex system composed of hundreds of species, and metaproteomics can be used to explore their expressed functions. However, many lower abundance species are not detected by current metaproteomic techniques and represent the dark field of metaproteomics. We do not know the minimal abundance of a bacterium in a microbiome(depth) that can be detected by shotgun metaproteomics. In this study, we spiked 15N-labeled E. coli peptides at different percentages into peptides mixture derived from the human gut microbiome to evaluate the depth that can be achieved by shotgun metaproteomics. We observed that the number of identified peptides and peptide intensity from 15N-labeled E. coli were linearly correlated with the spike-in levels even when 15N-labeled E. coli was down to 0.5% of the biomass. Below that level, it was not detected. Interestingly, the match-between-run strategy significantly increased the number of quantified peptides even when 15N-labeled E. coli peptides were at low abundance. This is indicative that in metaproteomics of complex gut microbiomes many peptides from low abundant species are likely observable in MS1 but are not selected for MS2 by standard shotgun strategies.
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