Using high-abundance proteins as guides for fast and effective peptide/protein identification from human gut metaproteomic data

Moses Stamboulian; Sujun Li; Yuzhen Ye

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Using high-abundance proteins as guides for fast and effective peptide/protein identification from human gut metaproteomic data

机译：Using high-abundance proteins as guides for fast and effective peptide/protein identification from human gut metaproteomic data

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BACKGROUND:A few recent large efforts significantly expanded the collection of human-associated bacterial genomes, which now contains thousands of entities including reference complete/draft genomes and metagenome assembled genomes (MAGs). These genomes provide useful resource for studying the functionality of the human-associated microbiome and their relationship with human health and diseases. One application of these genomes is to provide a universal reference for database search in metaproteomic studies, when matched metagenomic/metatranscriptomic data are unavailable. However, a greater collection of reference genomes may not necessarily result in better peptide/protein identification because the increase of search space often leads to fewer spectrum-peptide matches, not to mention the drastic increase of computation time. Video Abstract METHODS: Here, we present a new approach that uses two steps to optimize the use of the reference genomes and MAGs as the universal reference for human gut metaproteomic MS/MS data analysis. The first step is to use only the high-abundance proteins (HAPs) (i.e., ribosomal proteins and elongation factors) for metaproteomic MS/MS database search and, based on the identification results, to derive the taxonomic composition of the underlying microbial community. The second step is to expand the search database by including all proteins from identified abundant species. We call our approach HAPiID (HAPs guided metaproteomics IDentification).RESULTS:We tested our approach using human gut metaproteomic datasets from a previous study and compared it to the state-of-the-art reference database search method MetaPro-IQ for metaproteomic identification in studying human gut microbiota. Our results show that our two-steps method not only performed significantly faster but also was able to identify more peptides. We further demonstrated the application of HAPiID to revealing protein profiles of individual human-associated bacterial species, one or a few species at a time, using metaproteomic data.CONCLUSIONS:The HAP guided profiling approach presents a novel effective way for constructing target database for metaproteomic data analysis. The HAPiID pipeline built upon this approach provides a universal tool for analyzing human gut-associated metaproteomic data.

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《microbiome》 |2021年第1期|80-96|共17页
作者
Moses Stamboulian; Sujun Li; Yuzhen Ye;
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作者单位

Luddy School of Informatics, Computing and Engineering, Indiana University;

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正文语种英语
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Expanded target database; High-abundance protein (HAP); Human gut metaproteomics; Sample profiling; Spectra search;

Using high-abundance proteins as guides for fast and effective peptide/protein identification from human gut metaproteomic data

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