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A Universal Peptide Matrix Interactomics Approach to Disclose Motif-Dependent Protein Binding

Evelyn Ramberger, Lorena Suarez-Artiles, Daniel Pérez-Hernández, Mohamed Haji, Oliver Popp, Ulf Reimer, Achim Leutz, Gunnar Dittmar, Philipp Mertins

2021Molecular & Cellular Proteomics18 citationsDOIOpen Access PDF

Abstract

Protein-protein interactions mediated by intrinsically disordered regions are often based on short linear motifs (SLiMs). SLiMs are implicated in signal transduction and gene regulation yet remain technically laborious and notoriously challenging to study. Here, we present an optimized method for a protein interaction screen on a peptide matrix (PRISMA) in combination with quantitative MS. The protocol was benchmarked with previously described SLiM-based protein-protein interactions using peptides derived from EGFR, SOS1, GLUT1, and CEBPB and extended to map binding partners of kinase activation loops. The detailed protocol provides practical considerations for setting up a PRISMA screen and subsequently implementing PRISMA on a liquid-handling robotic platform as a cost-effective high-throughput method. Optimized PRISMA can be universally applied to systematically study SLiM-based interactions and associated post-translational modifications or mutations to advance our understanding of the largely uncharacterized interactomes of intrinsically disordered protein regions.

Topics & Concepts

Computational biologyProtein–protein interactionComputer sciencePeptideChemistryBiologyCell biologyBiochemistryAdvanced Proteomics Techniques and ApplicationsRNA and protein synthesis mechanismsGenomics and Chromatin Dynamics
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