Peptide-Centric Proteome Analysis: An Alternative Strategy for the Analysis of Tandem Mass Spectrometry Data

Ting, Ying S.; Egertson, Jarrett D.; Payne, Samuel H.; Kim, Sangtae; MacLean, Brendan; Käll, Lukas; Aebersold, Ruedi; Smith, Richard; Noble, William Stafford; MacCoss, Michael J.

doi:10.1074/mcp.o114.047035

Cited by 173 publications

(176 citation statements)

References 56 publications

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“…For example, Ting et al presented a perspective on spectrum-centric analysis versus peptide-centric analysis, the latter of which assesses the probability that a peptide is present without requiring a spectral library [47]. This ‘peptide-centric analysis’ has been implemented in the software PECAN, which tests directly for statistical probability that the query peptides are present [47]. Another tool recently introduced by our group makes use of uDIA and isotopic labeling to assess absolute stoichiometry of lysine acetylation and succinylation [53].…”

Section: Bioinformatic Resources For Analysis Of Data From Udiamentioning

confidence: 99%

Clinical applications of quantitative proteomics using targeted and untargeted data-independent acquisition techniques

Meyer

Schilling

2017

Expert Review of Proteomics

131

105

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Introduction While selected/multiple-reaction monitoring (SRM or MRM) is considered the gold standard for quantitative protein measurement, emerging data-independent acquisition (DIA) using high-resolution scans have opened a new dimension of high-throughput, comprehensive quantitative proteomics. These newer methodologies are particularly well suited for discovery of biomarker candidates from human disease samples, and for investigating and understanding human disease pathways. Areas covered This article reviews the current state of targeted and untargeted DIA mass spectrometry-based proteomic workflows, including SRM, parallel-reaction monitoring (PRM) and untargeted DIA (e.g., SWATH). Corresponding bioinformatics strategies, as well as application in biological and clinical studies are presented. Expert commentary Nascent application of highly-multiplexed untargeted DIA, such as SWATH, for accurate protein quantification from clinically relevant and disease-related samples shows great potential to comprehensively investigate biomarker candidates and understand disease.

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Section: Bioinformatic Resources For Analysis Of Data From Udiamentioning

confidence: 99%

Clinical applications of quantitative proteomics using targeted and untargeted data-independent acquisition techniques

Meyer

Schilling

2017

Expert Review of Proteomics

131

105

View full text Add to dashboard Cite

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“…Data‐independent acquisition (DIA) such as Sequential Window Acquisition of all Theoretical Fragment ion spectra (SWATH) forgo pre‐programmed precursor‐fragment pairs, widening the isolation windows to activate all ions in a pre‐specified mass‐to‐charge (m/z) range. A detailed review of DIA methodology can be found elsewhere, including peptide‐centric approaches to DIA . It is also possible, through MS1 filtering informatics techniques, to use data dependent acquisition (DDA) for quantitative analysis as opposed to conventional detection analysis.…”

Section: Introductionmentioning

confidence: 99%

The Skyline ecosystem: Informatics for quantitative mass spectrometry proteomics

Pino

Searle

Bollinger

et al. 2017

Mass Spectrometry Reviews

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Skyline is a freely available, open-source Windows client application for accelerating targeted proteomics experimentation, with an emphasis on the proteomics and mass spectrometry community as users and as contributors. This review covers the informatics encompassed by the Skyline ecosystem, from computationally assisted targeted mass spectrometry method development, to raw acquisition file data processing, and quantitative analysis and results sharing.

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“…However, methods for quantitative comparisons of site-specific protein glycoforms have only begun to emerge (9). While the comparative analysis of proteins by data independent acquisition (DIA) has improved the efficiency of quantitative proteomics analyses (20;21), applications of DIA methods to the analysis of posttranslational modifications are limited and virtually non-existent for glycoproteins (22). In this paper, we introduce a workflow for DIA analysis of N-glycopeptides under soft CID fragmentation conditions and document applicability of the glycopeptide DIA (Glycopeptide SWATH or GP-SWATH) workflow to the comparative analysis of fucosylated complex glycoforms of ten abundant plasma glycoprotein groups in the context of liver cirrhosis.…”

Section: Introductionmentioning

confidence: 99%

Site-specific analysis of changes in the glycosylation of proteins in liver cirrhosis using data-independent workflow with soft fragmentation

et al. 2016

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Cirrhosis of the liver is associated with increased fucosylation of proteins in the plasma. We describe a data independent (DIA) strategy for comparative analysis of the site-specific glycoforms of plasma glycoproteins. A library of 161 glycoforms of 25 N-glycopeptides was established by data dependent LC-MS/MS analysis of a tryptic digest of 14 human protein groups retained on a multiple affinity removal column. The collision induced dissociation conditions were adjusted to maximize the yield of selective Y-ions which were quantified by a data-independent mass spectrometry workflow using a 10 Da acquisition window. Using this workflow, we quantified 125 glycoforms of 25 glycopeptides, covering 10 of the 14 proteins, without any further glycopeptide enrichment. Comparison of the proteins in the plasma of healthy controls and cirrhotic patients shows an average 1.5 fold increase in the fucosylation of bi-antennary glycoforms and 3 fold increase in the fucosylation of tri- and tetra- antennary glycoforms. These results show that the adjusted glycopeptide DIA workflow using soft collision-induced fragmentation of glycopeptides is suitable for site specific analysis of protein glycosylation in complex mixtures of analytes without glycopeptide enrichment.

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Peptide-Centric Proteome Analysis: An Alternative Strategy for the Analysis of Tandem Mass Spectrometry Data

Cited by 173 publications

References 56 publications

Clinical applications of quantitative proteomics using targeted and untargeted data-independent acquisition techniques

Clinical applications of quantitative proteomics using targeted and untargeted data-independent acquisition techniques

The Skyline ecosystem: Informatics for quantitative mass spectrometry proteomics

Site-specific analysis of changes in the glycosylation of proteins in liver cirrhosis using data-independent workflow with soft fragmentation

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