Structure-based validation can drastically underestimate error rate in proteome-wide cross-linking mass spectrometry studies.

Kumar YugandharJean-Philippe Pellois Shayne D WierbowskiElnur Elyar ShayhidinHaiyuan Yu

Published in: Nature methods (2020)

Thorough quality assessment of novel interactions identified by proteome-wide cross-linking mass spectrometry (XL-MS) studies is critical. Almost all current XL-MS studies have validated cross-links against known three-dimensional structures of representative protein complexes. Here, we provide theoretical and experimental evidence demonstrating that this approach can drastically underestimate error rates for proteome-wide XL-MS datasets, and propose a comprehensive set of four data-quality metrics to address this issue.

Keyphrases

mass spectrometry
liquid chromatography
high resolution
gas chromatography
case control
capillary electrophoresis
multiple sclerosis
high performance liquid chromatography
ms ms
big data
machine learning
cross sectional
rna seq
tandem mass spectrometry
small molecule
amino acid
solid phase extraction