Ddi1 is a ubiquitin-dependent protease

Yip, M.C.J.; Bodnar, Nicholas O.; Rapoport, Tom A.

doi:10.1073/pnas.1902298117

Cited by 68 publications

(86 citation statements)

References 46 publications

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“…Intersects indicated in Figure 6A by arrows, are the subunits of the proteasome core, showing the strength of using mTPP in multiomics intersection analysis for identifying candidate protein subsets involved in the mechanism behind an observed phenotype. Aside from the core proteasome subunits, the additional member within this subset is the DNAdamage inducible protein 1 (Ddi1), a ubiquitin binding protein that functions as a proteasome shuttle (reviewed in (87)) that has recently been characterized as a ubiquitin-dependent protease (88). Ddi1 is destabilized in rpn5-ts as well (Supp.…”

Section: Multiomics Intersection Analysis Of Mtpp With Global Proteommentioning

confidence: 99%

Mutant thermal proteome profiling for characterization of missense protein variants and their associated phenotypes within the proteome

Justice

Barron

et al. 2020

Journal of Biological Chemistry

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Temperature sensitive (TS) missense mutants have been foundational for characterization of essentialgene function. However, an unbiased approach for analysis of biochemical and biophysical changes in TSmissense mutants within the context of their functional proteomes is lacking. We applied massspectrometry (MS) based thermal proteome profiling (TPP) to investigate the proteome-wide effects ofmissense mutations in an application that we refer to as mutant Thermal Proteome Profiling (mTPP).This study characterized global impacts of temperature sensitivity-inducing missense mutations in twodifferent subunits of the 26S proteasome. The majority of alterations identified by RNA-Seq and globalproteomics were similar between the mutants, which could suggest that a similar functional disruption isoccurring in both missense variants. Results from mTPP, however, provide unique insights into themechanisms that contribute to the TS phenotype in each mutant, revealing distinct changes that were notobtained using only steady-state transcriptome and proteome analyses. Computationally, multisite λ-dynamics simulations add clear support for mTPP experimental findings. This work shows that mTPP is aprecise approach to measure changes in missense mutant containing proteomes without the requirementfor large amounts of starting material, specific antibodies against proteins of interest, and/or geneticmanipulation of the biological system. Although experiments were performed under permissiveconditions, mTPP provided insights into the underlying protein stability changes that cause dramaticcellular phenotypes observed at non-permissive temperatures. Overall, mTPP provides uniquemechanistic insights into missense mutation dysfunction and connection of genotype to phenotype in arapid, non-biased fashion.

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Section: Multiomics Intersection Analysis Of Mtpp With Global Proteommentioning

confidence: 99%

Mutant thermal proteome profiling for characterization of missense protein variants and their associated phenotypes within the proteome

Justice

Barron

et al. 2020

Journal of Biological Chemistry

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“…When cells are challenged with an excess of DPCs, they may require an alternative DPC protease. Ddi1 and 26S proteasome could at least partially substitute for Wss1 function (Serbyn et al, 2020), and both of them target ubiquitinated proteins for degradation (Finley et al, 2012;Yip et al, 2020). Ubiquitin and SUMO are known to compete for the acceptor lysines (Hendriks et al, 2014).…”

Section: Deleterious Effects Of Siz2-dependent Sumo Conjugation On Tomentioning

confidence: 99%

SUMO orchestrates multiple alternative DNA-protein crosslink repair pathways

Serbyn

Bagdiul

Michel

et al. 2020

Preprint

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Several endogenous metabolites, environmental agents, and therapeutic drugs promote formation of covalent DNA-protein crosslinks (DPCs). Persistent DPCs pose a serious threat to genome integrity and are eliminated by multiple repair pathways. Aberrant Top1 crosslinks to DNA, or Top1ccs, are processed by Tdp1 and Wss1 functioning in parallel pathways in Saccharomyces cerevisiae. It remains obscure how cells choose between these diverse mechanisms of DPC repair. Here we show that several SUMO biogenesis factors -Ulp1, Siz2, Slx5, Slx8 -control repair of Top1cc or an analogous DPC lesion. Genetic analysis reveals that SUMO promotes Top1cc processing in the absence of Tdp1 but has an inhibitory role if cells additionally lack Wss1. In the tdp1D wss1D mutant, the E3 SUMO ligase Siz2 stimulates sumoylation in the vicinity of the DPC, but not SUMO conjugation to Top1. This Siz2-dependent sumoylation delays DPC repair when cells progress through S and G2 phases.Our findings suggest that SUMO tunes available repair pathways to facilitate faithful DPC repair.

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“…Indeed, it would in many ways make sense in the context of the role of Ddi1/DDI2 as ubiquitin shuttles if infrequent cleavage of long ubiquitin chains facilitated the loading into the proteasome of a large variety of proteins with long ubiquitin chains. Interestingly, while this manuscript was in revision, Rapoport and co-workers reported complementary data that showed that the yeast Ddi1 protein preferentially (or exclusively) recognizes an artificial target protein when it carries a long ubiquitin chain and that it may even weakly cut the chain itself ( Yip et al., 2020 ). Importantly, our results clearly indicate that proteins with very long ubiquitin chains are slowly degraded by the UPS and require DDI2 activity for their timely removal in vivo .…”

Section: Introductionmentioning

confidence: 99%

DDI2 Is a Ubiquitin-Directed Endoprotease Responsible for Cleavage of Transcription Factor NRF1

et al. 2020

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Summary The Ddi1/DDI2 proteins are ubiquitin shuttling factors, implicated in a variety of cellular functions. In addition to ubiquitin-binding and ubiquitin-like domains, they contain a conserved region with similarity to retroviral proteases, but whether and how DDI2 functions as a protease has remained unknown. Here, we show that DDI2 knockout cells are sensitive to proteasome inhibition and accumulate high-molecular weight, ubiquitylated proteins that are poorly degraded by the proteasome. These proteins are targets for the protease activity of purified DDI2. No evidence for DDI2 acting as a de-ubiquitylating enzyme was uncovered, which could suggest that it cleaves the ubiquitylated protein itself. In support of this idea, cleavage of transcription factor NRF1 is known to require DDI2 activity in vivo . We show that DDI2 is indeed capable of cleaving NRF1 in vitro but only when NRF1 protein is highly poly-ubiquitylated. Together, these data suggest that DDI2 is a ubiquitin-directed endoprotease.

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Ddi1 is a ubiquitin-dependent protease

Cited by 68 publications

References 46 publications

Mutant thermal proteome profiling for characterization of missense protein variants and their associated phenotypes within the proteome

Mutant thermal proteome profiling for characterization of missense protein variants and their associated phenotypes within the proteome

SUMO orchestrates multiple alternative DNA-protein crosslink repair pathways

DDI2 Is a Ubiquitin-Directed Endoprotease Responsible for Cleavage of Transcription Factor NRF1

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