Literature DB >> 29599191

AP-SWATH Reveals Direct Involvement of VCP/p97 in Integrated Stress Response Signaling Through Facilitating CReP/PPP1R15B Degradation.

Julia Hülsmann1, Bojana Kravic1, Matthias Weith1, Matthias Gstaiger2, Ruedi Aebersold2,3, Ben C Collins4, Hemmo Meyer5.   

Abstract

The ubiquitin-directed AAA-ATPase VCP/p97 facilitates degradation of damaged or misfolded proteins in diverse cellular stress response pathways. Resolving the complexity of its interactions with partner and substrate proteins and understanding its links to stress signaling is therefore a major challenge. Here, we used affinity-purification SWATH mass spectrometry (AP-SWATH) to identify proteins that specifically interact with the substrate-trapping mutant, p97-E578Q. AP-SWATH identified differential interactions over a large detection range from abundant p97 cofactors to pathway-specific partners and individual ligases such as RNF185 and MUL1 that were trapped in p97-E578Q complexes. In addition, we identified various substrate proteins and candidates including the PP1 regulator CReP/PPP1R15B that dephosphorylates eIF2α and thus counteracts attenuation of translation by stress-kinases. We provide evidence that p97 with its Ufd1-Npl4 adapter ensures rapid constitutive turnover and balanced levels of CReP in unperturbed cells. Moreover, we show that p97-mediated degradation, together with a reduction in CReP synthesis, is essential for timely stress-induced reduction of CReP levels and, consequently, for robust eIF2α phosphorylation to enforce the stress response. Thus, our results demonstrate that p97 not only facilitates bulk degradation of misfolded proteins upon stress, but also directly modulates the integrated stress response at the level of signaling.
© 2018 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  Chaperone*; Protein Degradation*; SWATH-MS; Stress response; Ubiquitin

Mesh:

Substances:

Year:  2018        PMID: 29599191      PMCID: PMC6030730          DOI: 10.1074/mcp.RA117.000471

Source DB:  PubMed          Journal:  Mol Cell Proteomics        ISSN: 1535-9476            Impact factor:   5.911


  62 in total

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8.  Molecular Mechanism of Substrate Processing by the Cdc48 ATPase Complex.

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9.  aLFQ: an R-package for estimating absolute protein quantities from label-free LC-MS/MS proteomics data.

Authors:  George Rosenberger; Christina Ludwig; Hannes L Röst; Ruedi Aebersold; Lars Malmström
Journal:  Bioinformatics       Date:  2014-04-20       Impact factor: 6.937

10.  G-actin provides substrate-specificity to eukaryotic initiation factor 2α holophosphatases.

Authors:  Ruming Chen; Cláudia Rato; Yahui Yan; Ana Crespillo-Casado; Hanna J Clarke; Heather P Harding; Stefan J Marciniak; Randy J Read; David Ron
Journal:  Elife       Date:  2015-03-16       Impact factor: 8.140

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Journal:  Mol Cell       Date:  2019-04-09       Impact factor: 17.970

2.  Interaction mapping of endoplasmic reticulum ubiquitin ligases identifies modulators of innate immune signalling.

Authors:  Emma J Fenech; Federica Lari; Philip D Charles; Roman Fischer; Marie Laétitia-Thézénas; Katrin Bagola; Adrienne W Paton; James C Paton; Mads Gyrd-Hansen; Benedikt M Kessler; John C Christianson
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3.  The ubiquitin-conjugating enzyme UBE2QL1 coordinates lysophagy in response to endolysosomal damage.

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4.  Mitochondrial MUL1 E3 ubiquitin ligase regulates Hypoxia Inducible Factor (HIF-1α) and metabolic reprogramming by modulating the UBXN7 cofactor protein.

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Review 5.  Order through destruction: how ER-associated protein degradation contributes to organelle homeostasis.

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6.  Target-Based Discovery of an Inhibitor of the Regulatory Phosphatase PPP1R15B.

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7.  CReP mediates selective translation initiation at the endoplasmic reticulum.

Authors:  Jonathan P Kastan; Elena Y Dobrikova; Jeffrey D Bryant; Matthias Gromeier
Journal:  Sci Adv       Date:  2020-06-03       Impact factor: 14.136

  7 in total

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