Quantitative mapping of proteasome interactomes and substrates using ProteasomeID

Author:

Bartolome Aleksandar1,Heiby Julia C1,Di Fraia Domenico1,Heinze Ivonne1,Knaudt Hannah1,Spaeth Ellen1ORCID,Omrani Omid1,Minetti Alberto1,Hofmann Maleen1,Kirkpatrick Joanna M1,Dau Therese1ORCID,Ori Alessandro1ORCID

Affiliation:

1. Leibniz Institute on Aging - Fritz Lipmann Institute

Abstract

Proteasomes are essential molecular machines responsible for the degradation of proteins in eukaryotic cells. Altered proteasome activity has been linked to neurodegeneration, auto-immune disorders and cancer. Despite the relevance for human disease and drug development, no method currently exists to monitor proteasome composition and interactions in vivo in animal models. To fill this gap, we developed a strategy based on tagging of proteasomes with promiscuous biotin ligases and generated a new mouse model enabling the quantification of proteasome interactions by mass spectrometry. We show that biotin ligases can be incorporated in fully assembled proteasomes without negative impact on their activity. We demonstrate the utility of our method by identifying novel proteasome-interacting proteins, charting interactomes across mouse organs, and showing that proximity-labeling enables the identification of both endogenous and small-molecule-induced proteasome substrates.

Funder

Deutsche Forschungsgemeinschaft

Else Kröner-Fresenius-Stiftung

Deutsches Zentrum für Herz-Kreislaufforschung

Fritz Thyssen Stiftung

Chan Zuckerberg Initiative

NCL Foundation

Publisher

eLife Sciences Publications, Ltd

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