Abstract
Multiple reaction monitoring (MRM) of peptides uses tandem mass spectrometry to quantify selected proteins of interest, such as those previously identified in differential studies. Using this technique, the specificity of precursor to product transitions is harnessed for quantitative analysis of multiple proteins in a single sample. The design of transitions is critical for the success of MRM experiments, but predicting signal intensity of peptides and fragmentation patterns ab initio is challenging given existing methods. The tool presented here, MRMaid (pronounced "mermaid") offers a novel alternative for rapid design of MRM transitions for the proteomics researcher. The program uses a combination of knowledge of the properties of optimal MRM transitions taken from expert practitioners and literature with MS/MS evidence derived from interrogation of a database of peptide identifications and their associated mass spectra. The tool also predicts retention time using a published model, allowing ordering of transition candidates. By exploiting available knowledge and resources to generate the most reliable transitions, this approach negates the need for theoretical prediction of fragmentation and the need to undertake prior "discovery" MS studies. MRMaid is a modular tool built around the Genome Annotating Proteomic Pipeline framework, providing a web-based solution with both descriptive and graphical visualizations of transitions. Predicted transition candidates are ranked based on a novel transition scoring system, and users may filter the results by selecting optional stringency criteria, such as omitting frequently modified residues, constraining the length of peptides, or omitting missed cleavages. Comparison with published transitions showed that MRMaid successfully predicted the peptide and product ion pairs in the majority of cases with appropriate retention time estimates. As the data content of the Genome Annotating Proteomic Pipeline repository increases, the coverage and reliability of MRMaid are set to increase further. MRMaid is freely available over the internet as an executable web-based service at www.mrmaid.info.
Highlights
Multiple reaction monitoring (MRM) of peptides uses tandem mass spectrometry to quantify selected proteins of interest, such as those previously identified in differential studies
Downloading Results from MRMaid—In the final output, MRMaid provides a tabulated list of ranked transition candidates, which are intended for validation using a mass spectrometry (MS) instrument
Retention Time—Elution time data are commonly used in combination with MS/MS to support transition design for MRM experiments [3, 12, 13]
Summary
The MRMaid method for transition design relies on the combination of two sources of information: first on prior knowledge of the kind of precursor peptides that generally perform better in MS/MS and second on mining the data in a proteomics data repository, Genome Annotating Proteomic Pipeline (GAPP) [19], to determine which precursor and corresponding fragment ions have appeared regularly for the given protein of interest. The proposed peptide candidates can be compared by downloading the page of MRMaid results and comparing RT and transition score (TS) values This process is explained below and allows users to design the optimal bespoke MRM experiment for their specific target proteins. The individual product ions are assessed in terms of signal intensity reproducibility: an average of signal intensity for the relevant m/z peaks is calculated across all applicable experiments as well as the variance and standard deviation values These descriptive statistics indicate the reproducibility of the fragment ions for a given precursor and point to the number of times one would expect to have to run the MRM experiment to observe a good result for the transition
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