Combining Precursor and Fragment Information for Improved Detection of Differential Abundance in Data Independent Acquisition

Huang, Ting; Bruderer, Roland; Muntel, Jan; Xuan, Yue; Vitek, Olga; Reiter, Lukas

doi:10.1074/mcp.ra119.001705

Cited by 48 publications

(49 citation statements)

References 40 publications

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“…With this methodology, Meier et al [57] detected more than 10 000 proteins in only 100 min with sensitivity into the low-attomolar range. While BoxCar approaches were originally developed to augment DDA scan types, the principle can also be applied to DIA [58].…”

Section: Improvements In Sample Separations and Throughputmentioning

confidence: 99%

Emerging mass spectrometry-based proteomics methodologies for novel biomedical applications

Pino

Rose

O’Broin

et al. 2020

Biochemical Society Transactions

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Research into the basic biology of human health and disease, as well as translational human research and clinical applications, all benefit from the growing accessibility and versatility of mass spectrometry (MS)-based proteomics. Although once limited in throughput and sensitivity, proteomic studies have quickly grown in scope and scale over the last decade due to significant advances in instrumentation, computational approaches, and bio-sample preparation. Here, we review these latest developments in MS and highlight how these techniques are used to study the mechanisms, diagnosis, and treatment of human diseases. We first describe recent groundbreaking technological advancements for MS-based proteomics, including novel data acquisition techniques and protein quantification approaches. Next, we describe innovations that enable the unprecedented depth of coverage in protein signaling and spatiotemporal protein distributions, including studies of post-translational modifications, protein turnover, and single-cell proteomics. Finally, we explore new workflows to investigate protein complexes and structures, and we present new approaches for protein–protein interaction studies and intact protein or top-down MS. While these approaches are only recently incipient, we anticipate that their use in biomedical MS proteomics research will offer actionable discoveries for the improvement of human health.

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Section: Improvements In Sample Separations and Throughputmentioning

confidence: 99%

Emerging mass spectrometry-based proteomics methodologies for novel biomedical applications

Pino

Rose

O’Broin

et al. 2020

Biochemical Society Transactions

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“…[118,119] DIA analysis can also benefit from incorporating MS2-level data in order to improve the accuracy of label-free quantification. [120] With isobaric labeling, peptides of each sample are covalently labeled with a sample-specific mass tag. Mass tags are comprised of a reporter ion, a balance group and a reactive group, which is usually an amine reactive group (NHS group) that binds to primary amines from the peptides.…”

Section: Control Of Biases At the Ms2-level Of Peptide Quantificationmentioning

confidence: 99%

Analyzing Ribosome Remodeling in Health and Disease

Petelski

Slavov

2020

Proteomics

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Increasing evidence suggests that ribosomes actively regulate protein synthesis. However, much of this evidence is indirect, leaving this layer of gene regulation largely unexplored, in part due to methodological limitations. Indeed, evidence is reviewed demonstrating that commonly used methods, such as transcriptomics, are inadequate because the variability in mRNAs coding for ribosomal proteins (RP) does not necessarily correspond to RP variability. Thus protein remodeling of ribosomes should be investigated by methods that allow direct quantification of RPs, ideally of isolated ribosomes. Such methods are reviewed, focusing on mass spectrometry and emphasizing method‐specific biases and approaches to control these biases. It is argued that using multiple complementary methods can help reduce the danger of interpreting reproducible systematic biases as evidence for ribosome remodeling.

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“…This allows each phosphopeptide to be quantified from its MS1 precursor ion signal. It should be noted that, although not every phosphopeptide may have been subjected to MS2 fragmentation in each sample, it still remains quantifiable [ 152 , 154 , 155 , 156 ].…”

Section: Strategies For the Identification Of The Protein Kinase Tmentioning

confidence: 99%

Phosphoproteomics Meets Chemical Genetics: Approaches for Global Mapping and Deciphering the Phosphoproteome

Jurcik

Siváková

Cipakova

et al. 2020

IJMS

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Protein kinases are important enzymes involved in the regulation of various cellular processes. To function properly, each protein kinase phosphorylates only a limited number of proteins among the thousands present in the cell. This provides a rapid and dynamic regulatory mechanism that controls biological functions of the proteins. Despite the importance of protein kinases, most of their substrates remain unknown. Recently, the advances in the fields of protein engineering, chemical genetics, and mass spectrometry have boosted studies on identification of bona fide substrates of protein kinases. Among the various methods in protein kinase specific substrate identification, genetically engineered protein kinases and quantitative phosphoproteomics have become promising tools. Herein, we review the current advances in the field of chemical genetics in analog-sensitive protein kinase mutants and highlight selected strategies for identifying protein kinase substrates and studying the dynamic nature of protein phosphorylation.

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Combining Precursor and Fragment Information for Improved Detection of Differential Abundance in Data Independent Acquisition

Cited by 48 publications

References 40 publications

Emerging mass spectrometry-based proteomics methodologies for novel biomedical applications

Emerging mass spectrometry-based proteomics methodologies for novel biomedical applications

Analyzing Ribosome Remodeling in Health and Disease

Phosphoproteomics Meets Chemical Genetics: Approaches for Global Mapping and Deciphering the Phosphoproteome

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