Valosin-containing protein (VCP)–Adaptor Interactions are Exceptionally Dynamic and Subject to Differential Modulation by a VCP Inhibitor

Xue, Liang; Blythe, Emily E.; Freiberger, Elyse C.; Mamrosh, Jennifer L.; Hebert, Alexander S.; Reitsma, Justin M.; Hess, Sonja; Coon, Joshua J.; Deshaies, Raymond J.

doi:10.1074/mcp.m116.061036

Cited by 44 publications

(49 citation statements)

References 68 publications

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“…Our evidence based on dominant-negative VCP/p97 and two distinct VCP/p97 inhibitors ( Figure 6 ) implicates this ATPase in the Wnt-dependent inactivation of Ub-TLE. Intriguingly, a recent proteomic screen for NMS-873-induced VCP/p97-associated proteins identified TLE1 and TLE3 as the only Wnt signaling components, along with VCP/p97 adaptors and other putative substrates ( Xue et al., 2016 ), consistent with our notion of Groucho/TLE as a substrate of this ATPase. VCP/p97 regulates the folding of ubiquitylated proteins, to promote their segregation from large structures, such as endomembranes, and also from large protein complexes, including DNA repair and chromatin complexes ( Dantuma et al., 2014 , Xia et al., 2016 ).…”

Section: Discussionsupporting

confidence: 86%

Wnt-Dependent Inactivation of the Groucho/TLE Co-repressor by the HECT E3 Ubiquitin Ligase Hyd/UBR5

et al. 2017

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SummaryExtracellular signals are transduced to the cell nucleus by effectors that bind to enhancer complexes to operate transcriptional switches. For example, the Wnt enhanceosome is a multiprotein complex associated with Wnt-responsive enhancers through T cell factors (TCF) and kept silent by Groucho/TLE co-repressors. Wnt-activated β-catenin binds to TCF to overcome this repression, but how it achieves this is unknown. Here, we discover that this process depends on the HECT E3 ubiquitin ligase Hyd/UBR5, which is required for Wnt signal responses in Drosophila and human cell lines downstream of activated Armadillo/β-catenin. We identify Groucho/TLE as a functionally relevant substrate, whose ubiquitylation by UBR5 is induced by Wnt signaling and conferred by β-catenin. Inactivation of TLE by UBR5-dependent ubiquitylation also involves VCP/p97, an AAA ATPase regulating the folding of various cellular substrates including ubiquitylated chromatin proteins. Thus, Groucho/TLE ubiquitylation by Hyd/UBR5 is a key prerequisite that enables Armadillo/β-catenin to activate transcription.

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Section: Discussionsupporting

confidence: 86%

Wnt-Dependent Inactivation of the Groucho/TLE Co-repressor by the HECT E3 Ubiquitin Ligase Hyd/UBR5

et al. 2017

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“…We next asked whether they can bind p97 at the same time and therefore first analyzed proteins co‐immunoprecipitating with UBXD1. Because p97‐cofactor complexes can dissociate quickly after cell lysis (Xue et al , ), we used stable cells expressing the ATPase‐deficient trapping mutant p97‐E578Q (p97‐EQ) at near endogenous levels in addition to p97‐wt cells. Indeed, UBXD1 co‐precipitated p97 and also co‐isolated PLAA in the p97‐EQ background (Fig D).…”

Section: Resultsmentioning

confidence: 99%

VCP /p97 cooperates with YOD 1, UBXD 1 and PLAA to drive clearance of ruptured lysosomes by autophagy

et al. 2016

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Rupture of endosomes and lysosomes is a major cellular stress condition leading to cell death and degeneration. Here, we identified an essential role for the ubiquitin-directed AAA-ATPase, p97, in the clearance of damaged lysosomes by autophagy. Upon damage, p97 translocates to lysosomes and there cooperates with a distinct set of cofactors including UBXD1, PLAA, and the deubiquitinating enzyme YOD1, which we term ELDR components for Endo-Lysosomal Damage Response. Together, they act downstream of K63-linked ubiquitination and p62 recruitment, and selectively remove K48-linked ubiquitin conjugates from a subpopulation of damaged lysosomes to promote autophagosome formation. Lysosomal clearance is also compromised in MEFs harboring a p97 mutation that causes inclusion body myopathy and neurodegeneration, and damaged lysosomes accumulate in affected patient tissue carrying the mutation. Moreover, we show that p97 helps clear late endosomes/lysosomes ruptured by endocytosed tau fibrils. Thus, our data reveal an important mechanism of how p97 maintains lysosomal homeostasis, and implicate the pathway as a modulator of degenerative diseases.

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“…It is unclear whether post-lysis SR exchange is a problem for other CRL complexes, but we suspect that it is considering that Cand1 binds other cullins (Bennett et al, 2010; Chua et al, 2011; Liu et al, 2002; Min et al, 2003; Zheng et al, 2002). Although SR exchange is a facilitated process, in the case of the p97 network rapid equilibration of cofactors is mediated by their high intrinsic k on and k off (Xue et al, 2016). This problem is likely to be widespread and may affect other heteromeric enzymes that undergo dynamic remodeling, like protein phosphatase 2A (Kong et al, 2009).…”

Section: Discussionmentioning

confidence: 99%

Composition and Regulation of the Cellular Repertoire of SCF Ubiquitin Ligases

Reitsma

Liu

Reichermeier

et al. 2017

Cell

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124

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Summary SCF (Skp1-Cullin-F-box) ubiquitin ligases comprise several dozen modular enzymes that have diverse roles in biological regulation. SCF enzymes share a common catalytic core containing Cul1•Rbx1, which is directed towards different substrates by a variable substrate receptor (SR) module comprising one of 69 F-box proteins bound to Skp1. Despite the broad cellular impact of SCF enzymes, important questions remain about the architecture and regulation of the SCF repertoire, including whether SRs compete for Cul1, and if so, how this competition is managed. Here, we devise methods that preserve the in vivo assemblages of SCF complexes, and apply quantitative mass spectrometry to perform a census of these complexes (the ‘SCFome’) in various states. We show that Nedd8 conjugation and the SR exchange factor Cand1 have a profound effect on shaping the SCFome. Together, these factors enable rapid remodeling of SCF complexes to promote biased assembly of SR modules bound to substrate.

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Valosin-containing protein (VCP)–Adaptor Interactions are Exceptionally Dynamic and Subject to Differential Modulation by a VCP Inhibitor

Cited by 44 publications

References 68 publications

Wnt-Dependent Inactivation of the Groucho/TLE Co-repressor by the HECT E3 Ubiquitin Ligase Hyd/UBR5

Wnt-Dependent Inactivation of the Groucho/TLE Co-repressor by the HECT E3 Ubiquitin Ligase Hyd/UBR5

VCP /p97 cooperates with YOD 1, UBXD 1 and PLAA to drive clearance of ruptured lysosomes by autophagy

Composition and Regulation of the Cellular Repertoire of SCF Ubiquitin Ligases

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