2023
DOI: 10.1038/s41589-023-01388-1
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Molecular basis for ubiquitin/Fubi cross-reactivity in USP16 and USP36

Rachel O’Dea,
Nafizul Kazi,
Alicia Hoffmann-Benito
et al.

Abstract: Ubiquitin and ubiquitin-like proteins typically use distinct machineries to facilitate diverse functions. The immunosuppressive ubiquitin-like protein Fubi is synthesized as an N-terminal fusion to a ribosomal protein (Fubi-S30). Its proteolytic maturation by the nucleolar deubiquitinase USP36 is strictly required for translationally competent ribosomes. What endows USP36 with this activity, how Fubi is recognized and whether other Fubi proteases exist are unclear. Here, we report a chemical tool kit that faci… Show more

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Cited by 9 publications
(9 citation statements)
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“…We therefore turned to the Ubl Fubi which like ubiquitin is synthesized as an N-terminal fusion to a ribosomal protein (Fubi-S30) and cleaved by the nucleolar DUB USP36 to release free Fubi and S30 . In addition to USP36, the mainly cytosolic DUB USP16 has Fubi protease activity, which may give rise to a two-tier system of Fubi-S30 maturation . In immune cells, Fubi conveys immunosuppressive signaling, including suppression of the maternal immune system upon embryo implantation, and isopeptide-linked conjugates of Fubi have been observed for selected proteins (termed Fubiylation in analogy to Ubiquitylation). , However, which enzymes can act as deFubiylases with the ability to specifically antagonize these isopeptide-linked Fubi conjugates is not known.…”
Section: Resultsmentioning
confidence: 99%
See 2 more Smart Citations
“…We therefore turned to the Ubl Fubi which like ubiquitin is synthesized as an N-terminal fusion to a ribosomal protein (Fubi-S30) and cleaved by the nucleolar DUB USP36 to release free Fubi and S30 . In addition to USP36, the mainly cytosolic DUB USP16 has Fubi protease activity, which may give rise to a two-tier system of Fubi-S30 maturation . In immune cells, Fubi conveys immunosuppressive signaling, including suppression of the maternal immune system upon embryo implantation, and isopeptide-linked conjugates of Fubi have been observed for selected proteins (termed Fubiylation in analogy to Ubiquitylation). , However, which enzymes can act as deFubiylases with the ability to specifically antagonize these isopeptide-linked Fubi conjugates is not known.…”
Section: Resultsmentioning
confidence: 99%
“…To address these shortcomings, we developed individual synthesis and purification protocols for the generation of fully folded isopeptide-linked fluorescence polarization substrates based on Ubl C-terminal acyl azides. We confirm the complete conversion of a suite of Ub/Ubl-KG-TAMRA reagents in enzymatic assays and apply it to the quantification of Ub/Ubl cross-reactivity of various DUBs including the recently identified Fubi proteases USP16 and USP36, , which we show to be the first trispecific Ubl isopeptidase with previously overlooked deISGylation activity. Moreover, we focused on recently structurally characterized USPL1 (Figure D), which is the only deSUMOylase with a USP fold but for which its mechanism for SUMO paralogue specificity had remained unclear.…”
Section: Introductionmentioning
confidence: 99%
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“…As serine is highly efficient at forming H-bonds, it could be that this serine is the critical residue of choice in USP16 and USP45 as well. Recently, cellular USP45 was shown to display elevated reactivity towards protein probes, not in line with its in vitro catalytic activity, which stresses that serine as the third catalytic residue does not coincide with lower nucleophilicity (O'Dea et al, 2023).…”
Section: Discussionmentioning
confidence: 99%
“…USP18 is predominantly the deISGylase thought to act in cells particularly as its expression aligns with the interferon response and ISG15 . Other USP-family members such as USP5, USP14, USP16, USP21, and USP36 [ 277 , 287 ], have all shown deISGylase activity in vitro on top of their primary protease activity against other UBLs and/or Ub. Whether these moonlighting activities are relevant to ISG15 biology remains to be seen, but the development of specific tools to probe activity in response to DNA damage will likely aid future work.…”
Section: Ulps In Genome Stabilitymentioning
confidence: 99%