Active site alanine mutations convert deubiquitinases into high‐affinity ubiquitin‐binding proteins

Morrow, Marie E.; Morgan, Michael T.; Clerici, Marcello; Growková, Kateřina; Yan, Ming; Komander, David; Sixma, Titia K.; Šimíček, Michal; Wolberger, Cynthia

doi:10.15252/embr.201745680

Cited by 44 publications

(39 citation statements)

References 49 publications

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“…Indeed, N12A mutation of UCHL3 decreased its affinity for K27 diUb by 80 %( Supporting Information, Figure S10). Note that C95A mutation of UCHL3 was previously reported to enhance its binding to mono-Ub [29,30] (Supporting Information, Figure S11), but for K27 diUb this enhancement effect was not observed in our ITC and pull-down experiments (Supporting Information, Figure S12). However,the binding affinity of the C95A mutant to other diUb chains was found to be increased (Supporting Information, Figure S12).…”

Section: Zuschriftenmentioning

confidence: 62%

Chemical Protein Synthesis Enabled Mechanistic Studies on the Molecular Recognition of K27‐linked Ubiquitin Chains

et al. 2019

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New synthetic strategies that exploited the strengths of both chemoselective ligation and recombinant protein expression were developed to prepare K27 di-ubiquitins (diUb), which enabled mechanistic studies on the molecular recognition of K27-linked Ubs by single-molecule Fçrster resonance energy transfer (smFRET) and X-ray crystallography.The results revealed that free K27 diUb adopted acompact conformation, whereas upon binding to UCHL3, K27 diUb was remodeled to an open conformation. The K27 isopeptide bond remained rigidly buried inside the diUb moiety during binding,a ni nteresting unique structural feature that may explain the distinctive biological function of K27 Ub chains.

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Section: Zuschriftenmentioning

confidence: 62%

Chemical Protein Synthesis Enabled Mechanistic Studies on the Molecular Recognition of K27‐linked Ubiquitin Chains

et al. 2019

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“…Related to this, avidity-based, high-affinity protein binders specific for free ubiquitin have been engineered that are useful as sensors for free mono-ubiquitin levels 53 . Recent work has also shown that Cys-to-Ala mutation within some DUB catalytic triads results in highaffinity ubiquitin binding that could be used similarly 54 . To analyze OtDUB for this potential, we tested mono-ubiquitin binding by ITC to OtDUB 1-177 bearing a C135A mutation, but saw only weak binding (K d = 6.3 ± 0.2 µM, n = 1.8 ± 0.04) (Supplementary Fig.…”

Section: Discussionmentioning

confidence: 99%

A deubiquitylase with an unusually high-affinity ubiquitin-binding domain from the scrub typhus pathogen Orientia tsutsugamushi

et al. 2020

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Ubiquitin mediated signaling contributes critically to host cell defenses during pathogen infection. Many pathogens manipulate the ubiquitin system to evade these defenses. Here we characterize a likely effector protein bearing a deubiquitylase (DUB) domain from the obligate intracellular bacterium Orientia tsutsugamushi, the causative agent of scrub typhus. The Ulp1like DUB prefers ubiquitin substrates over ubiquitin-like proteins and efficiently cleaves polyubiquitin chains of three or more ubiquitins. The co-crystal structure of the DUB (OtDUB) domain with ubiquitin revealed three bound ubiquitins: one engages the S1 site, the second binds an S2 site contributing to chain specificity and the third binds a unique ubiquitin-binding domain (UBD). The UBD modulates OtDUB activity, undergoes a pronounced structural transition upon binding ubiquitin, and binds monoubiquitin with an unprecedented~5 nM dissociation constant. The characterization and high-resolution structure determination of this enzyme should aid in its development as a drug target to counter Orientia infections.

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“…Affinity might be increased, as noted above, with either modified linkers or alternative UBDs. Our designs have utilized only a few of more than 20 types of UBDs 44,45 ; moreover, other Ub binding proteins such as catalyticallyinactive DUBs might be used as components of tUBD-type fusion constructs 46 .…”

Section: Discussionmentioning

confidence: 99%

High-affinity free ubiquitin sensors as quantitative probes of ubiquitin homeostasis and deubiquitination

Choi

Bollinger

Prada

et al. 2019

Preprint

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Ubiquitin (Ub) conjugation is an essential post-translational modification that affects nearly all proteins in eukaryotes. The functions and mechanisms of ubiquitination are areas of extensive and ongoing study, and yet the dynamics and regulation of even free (i.e., unconjugated) Ub are poorly understood. A major impediment has been the lack of simple and robust techniques to quantify Ub levels in cells and to monitor Ub release from conjugates. Here we describe the development of avidity-based fluorescent sensors that address this need. The sensors bind specifically to free Ub, have K d values down to 60 pM, and, in concert with a newly developed workflow, allow us to distinguish and quantify the pools of free, protein-conjugated, and thioesterified forms of Ub from cell lysates. Alternatively, free Ub in fixed cells can be visualized microscopically by staining with a sensor. Real-time assays using the sensors afford unprecedented flexibility and precision to measure deubiquitination of virtually any (poly)Ub conjugate.

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Active site alanine mutations convert deubiquitinases into high‐affinity ubiquitin‐binding proteins

Cited by 44 publications

References 49 publications

Chemical Protein Synthesis Enabled Mechanistic Studies on the Molecular Recognition of K27‐linked Ubiquitin Chains

Chemical Protein Synthesis Enabled Mechanistic Studies on the Molecular Recognition of K27‐linked Ubiquitin Chains

A deubiquitylase with an unusually high-affinity ubiquitin-binding domain from the scrub typhus pathogen Orientia tsutsugamushi

High-affinity free ubiquitin sensors as quantitative probes of ubiquitin homeostasis and deubiquitination

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