AI Article Synopsis

  • Traditional database search methods for analyzing mass spectrometry data struggle to detect peptides with post-translational modifications (PTMs), leading to a rise in "open modification" search strategies that allow for more flexibility in mass matching.
  • A study by Kong highlighted that the open modification search tool MSFragger may be better at detecting peptides compared to traditional "narrow window" searches, prompting an empirical investigation into this claim.
  • The investigation revealed potential issues with false discovery rate (FDR) control in certain machine learning tools, but upon reanalysis with standard FDR control methods, it was found that concerns about their reliability in proteomics MS/MS searches may not be substantiated.

Article Abstract

Traditional database search methods for the analysis of bottom-up proteomics tandem mass spectrometry (MS/MS) data are limited in their ability to detect peptides with post-translational modifications (PTMs). Recently, "open modification" database search strategies, in which the requirement that the mass of the database peptide closely matches the observed precursor mass is relaxed, have become popular as ways to find a wider variety of types of PTMs. Indeed, in one study, Kong reported that the open modification search tool MSFragger can achieve higher statistical power to detect peptides than a traditional "narrow window" database search. We investigated this claim empirically and, in the process, uncovered a potential general problem with false discovery rate (FDR) control in the machine learning postprocessors Percolator and PeptideProphet. This problem might have contributed to Kong 's report that their empirical results suggest that false discovery (FDR) control in the narrow window setting might generally be compromised. Indeed, reanalyzing the same data while using a more standard form of target-decoy competition-based FDR control, we found that, after accounting for chimeric spectra as well as for the inherent difference in the number of candidates in open and narrow searches, the data does not provide sufficient evidence that FDR control in proteomics MS/MS database search is inherently problematic.

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Source
http://dx.doi.org/10.1021/acs.jproteome.3c00902DOI Listing

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