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Global profiling of protein complex dynamics with an experimental library of protein interaction markers

Christian Doerig, Cathy Marulli, Thomas R. Peskett, Norbert Volkmar, Lorenzo Pantolini, Gabriel Studer, Camilla Paleari, Fabian Frommelt, Torsten Schwede, Natalie de Souza, Yves Barral, Paola Picotti

2024Nature Biotechnology14 citationsDOIOpen Access PDF

Abstract

Methods to systematically monitor protein complex dynamics are needed. We introduce serial ultrafiltration combined with limited proteolysis-coupled mass spectrometry (FLiP-MS), a structural proteomics workflow that generates a library of peptide markers specific to changes in PPIs by probing differences in protease susceptibility between complex-bound and monomeric forms of proteins. The library includes markers mapping to protein-binding interfaces and markers reporting on structural changes that accompany PPI changes. Integrating the marker library with LiP-MS data allows for global profiling of protein-protein interactions (PPIs) from unfractionated lysates. We apply FLiP-MS to Saccharomyces cerevisiae and probe changes in protein complex dynamics after DNA replication stress, identifying links between Spt-Ada-Gcn5 acetyltransferase activity and the assembly state of several complexes. FLiP-MS enables protein complex dynamics to be probed on any perturbation, proteome-wide, at high throughput, with peptide-level structural resolution and informing on occupancy of binding interfaces, thus providing both global and molecular views of a system under study.

Topics & Concepts

ProteomeProteomicsComputational biologyProtein dynamicsProteaseProtein–protein interactionChemistrySaccharomyces cerevisiaePlasma protein bindingPeptideProtein structureBiologyBiochemistryYeastEnzymeGeneProtein Structure and DynamicsFungal and yeast genetics researchEnzyme Structure and Function
Global profiling of protein complex dynamics with an experimental library of protein interaction markers | Litcius