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Ubiquitin-independent proteasomal degradation driven by C-degron pathways.

Molecular cell (2023-05-19)
Yaara Makaros, Anat Raiff, Richard T Timms, Ajay R Wagh, Mor Israel Gueta, Aizat Bekturova, Julia Guez-Haddad, Sagie Brodsky, Yarden Opatowsky, Michael H Glickman, Stephen J Elledge, Itay Koren
ZUSAMMENFASSUNG

Although most eukaryotic proteins are targeted for proteasomal degradation by ubiquitination, a subset have been demonstrated to undergo ubiquitin-independent proteasomal degradation (UbInPD). However, little is known about the molecular mechanisms driving UbInPD and the degrons involved. Utilizing the GPS-peptidome approach, a systematic method for degron discovery, we found thousands of sequences that promote UbInPD; thus, UbInPD is more prevalent than currently appreciated. Furthermore, mutagenesis experiments revealed specific C-terminal degrons required for UbInPD. Stability profiling of a genome-wide collection of human open reading frames identified 69 full-length proteins subject to UbInPD. These included REC8 and CDCA4, proteins which control proliferation and survival, as well as mislocalized secretory proteins, suggesting that UbInPD performs both regulatory and protein quality control functions. In the context of full-length proteins, C termini also play a role in promoting UbInPD. Finally, we found that Ubiquilin family proteins mediate the proteasomal targeting of a subset of UbInPD substrates.

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Sigma-Aldrich
DAPI, for nucleic acid staining
Sigma-Aldrich
Monoklonaler Anti-Vinculin-Antikörper in Maus hergestellte Antikörper, clone hVIN-1, ascites fluid
Sigma-Aldrich
DUB-Inhibitor V, PR-619, Calbiochem, The DUB Inhibitor V, PR-619 controls the biological activity of DUB. This small molecule/inhibitor is primarily used for Protease Inhibitors applications.