| Literature DB >> 26412692 |
Kira Vyatkina1,2, Si Wu3, Lennard J M Dekker4, Martijn M VanDuijn4, Xiaowen Liu5,6, Nikola Tolić7, Mikhail Dvorkin1, Sonya Alexandrova1, Theo M Luider4, Ljiljana Paša-Tolić7, Pavel A Pevzner2,8.
Abstract
De novo sequencing of proteins and peptides is one of the most important problems in mass spectrometry-driven proteomics. A variety of methods have been developed to accomplish this task from a set of bottom-up tandem (MS/MS) mass spectra. However, a more recently emerged top-down technology, now gaining more and more popularity, opens new perspectives for protein analysis and characterization, implying a need for efficient algorithms to process this kind of MS/MS data. Here, we describe a method that allows for the retrieval, from a set of top-down MS/MS spectra, of long and accurate sequence fragments of the proteins contained in the sample. To this end, we outline a strategy for generating high-quality sequence tags from top-down spectra, and introduce the concept of a T-Bruijn graph by adapting to the case of tags the notion of an A-Bruijn graph widely used in genomics. The output of the proposed approach represents the set of amino acid strings spelled out by optimal paths in the connected components of a T-Bruijn graph. We illustrate its performance on top-down data sets acquired from carbonic anhydrase 2 (CAH2) and the Fab region of alemtuzumab.Entities:
Keywords: T-Bruijn graph; de novo sequencing; top-down mass spectrometry
Mesh:
Substances:
Year: 2015 PMID: 26412692 DOI: 10.1021/pr501244v
Source DB: PubMed Journal: J Proteome Res ISSN: 1535-3893 Impact factor: 4.466