Literature DB >> 22804252

MRMaid 2.0: mining PRIDE for evidence-based SRM transitions.

Jun Fan1, Fady Mohareb, Nicholas J Bond, Kathryn S Lilley, Conrad Bessant.   

Abstract

Selected reaction monitoring (SRM) is becoming the tool of choice for targeted quantitative proteomics. The fundamental principle of proteomic SRM is that, for a given protein of interest, there is a set of peptides that are unique to that protein. The characteristic retention time (RT), and intact peptide m/z of these so-called proteotypic peptides are then programmed into the mass spectrometer, along with the m/z of high-intensity product ions for targeted quantitation. The particular combination of RT, peptide m/z, and product m/z for a given peptide is referred to as a transition. Selection of the most appropriate set of transitions for a given set of proteins is crucial to any SRM experiment. We previously developed the web-based MRMaid tool, which suggested the optimal transitions for a given human protein by mining spectral evidence from a small in-house database. In this article we present a completely new implementation of MRMaid, which offers substantial improvements over the original. The new version, MRMaid 2.0, uses spectra from the EBI's PRIDE database, which massively increases the coverage and quality of transitions. Transition lists can now be generated for multiple proteins simultaneously, edited within the web browser, and exported for laboratory use.

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Year:  2012        PMID: 22804252      PMCID: PMC3437039          DOI: 10.1089/omi.2011.0143

Source DB:  PubMed          Journal:  OMICS        ISSN: 1536-2310


  17 in total

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5.  The development of multiple reaction monitoring assays for liver-derived plasma proteins.

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6.  Use of multiple reaction monitoring for multiplex analysis of colorectal cancer-associated proteins in human feces.

Authors:  Ching-Seng Ang; Julie Rothacker; Heather Patsiouras; Peter Gibbs; Antony W Burgess; Edouard C Nice
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7.  A guide to the Proteomics Identifications Database proteomics data repository.

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9.  A high-confidence human plasma proteome reference set with estimated concentrations in PeptideAtlas.

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  8 in total

1.  Bioinformatics challenges and solutions in proteomics as quantitative methods mature.

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Review 3.  Application of targeted mass spectrometry in bottom-up proteomics for systems biology research.

Authors:  Nathan P Manes; Aleksandra Nita-Lazar
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Review 4.  Making proteomics data accessible and reusable: current state of proteomics databases and repositories.

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5.  Pride-asap: automatic fragment ion annotation of identified PRIDE spectra.

Authors:  Niels Hulstaert; Florian Reisinger; Jonathan Rameseder; Harald Barsnes; Juan Antonio Vizcaíno; Lennart Martens
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Review 6.  Open source libraries and frameworks for mass spectrometry based proteomics: a developer's perspective.

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7.  2016 update of the PRIDE database and its related tools.

Authors:  Juan Antonio Vizcaíno; Attila Csordas; Noemi del-Toro; José A Dianes; Johannes Griss; Ilias Lavidas; Gerhard Mayer; Yasset Perez-Riverol; Florian Reisinger; Tobias Ternent; Qing-Wei Xu; Rui Wang; Henning Hermjakob
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Review 8.  Exploring the potential of public proteomics data.

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  8 in total

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