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Structural characterization of human Uch37

Journal Article · · Proteins
DOI:https://doi.org/10.1002/prot.23147· OSTI ID:1034961
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Uch37 is a deubiquitylating enzyme (DUB) that is functionally linked with multiple protein complexes and signal transduction pathways. Uch37 associates with the 26S proteasome through Rpn13 where it serves to remove distal ubiquitin moeities from polyubiquitylated proteins. Uch37's proteasome associated activity was shown to liberate proteins from destruction. However, Uch37 may also specifically facilitate the destruction of inducible nitric oxide synthase and I{kappa}B-{alpha} at the proteasome. Wicks et al. established Uch37's potential to modulate the transforming growth factor-{beta}(TGF-{beta}) signaling cascade, through tis interaction with SMAD7. Yao et al. demonstrated that Uch37 also associates with the Ino80 chromatin-remodeling complex (Ino80 complex), which is involved in DNA repair and transcriptional regulation. Uch37's importance in metazoan development was underscored recently as Uch37 knockouts in mice result in prenatal lethality, where mutant embryos had severe defects in brain development. Protein ubiquitylation is an ATP-dependent post-translational modification that serves to signal a wide variety of cellular processes in eukaryotes. A protein cascade, generally comprising three enzymes, functions to activate, transport and specifically transfer ubiquitin to the targeted protein, culminating in an isopeptide linkage between the {epsilon}-amino group of a target protein's lysysl residue and the ubiquitin's terminal carboxylate. Monoubiquitination plays an important role in histone regulation, endocytosis, and viral budding. Further processing of the target protein may be accomplished by ubiquitylation of the protein on a different lysine, or through the formation of polyubiquitin chains, where the best-characterized outcome is destruction of the polyubiquitin-labeled protein in the proteasome. DUBs catalyze the removal of ubiquitin from proteins. This activity serves to reverse the effects of ubiquitination, permit ubiquitin recycling, or liberate free ubiquitin after translation. Uch37, is a cysteine protease from the ubiquitin C-terminal hydrolase (UCH) family. The catalytic domain of UCH enzymes has a central, six-stranded, antiparallel {beta}-sheet that is flanked on each side by {alpha}-helices. Like picornain 3C, UCH family proteins contain a catalytic triad comprising the side chains of cysteine, histidine, and aspartate. in picornain 3C, the aspartate's carboxylate side chain acts to position histidine's imidazole group for general base catalysis, which activates cysteine for nucleophilic attack. UCH enzymes also contain a glutamine, which may serve to stabilize the tetrahedral transition state. The UCH family can be divided into two distinct groups, that is, enzymes solely composed of the globular UCH fold, or enzymes comprising the UCH domain and a C-terminal extension. The latter group can be subdivided based on the composition of the C-terminal extension. Uch37 carries a C-terminal extension. Until now, the structure of a full-length UCH from this structural class has not been reported.
Research Organization:
Advanced Photon Source (APS), Argonne National Laboratory (ANL), Argonne, IL (US)
Sponsoring Organization:
NSFOTHERDOE - BASIC ENERGY SCIENCESNIHOTHER U.S. STATESNCI
OSTI ID:
1034961
Journal Information:
Proteins, Journal Name: Proteins Journal Issue: (2) ; 02, 2012 Vol. 80; ISSN PSFGEY; ISSN 0887-3585
Country of Publication:
United States
Language:
ENGLISH

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Related Subjects

59 BASIC BIOLOGICAL SCIENCES
60 APPLIED LIFE SCIENCES
BRAIN
CATALYSIS
CYSTEINE
DEFECTS
DNA REPAIR
EMBRYOS
ENZYMES
GLUTAMINE
HISTIDINE
HISTONES
HYDROLASES
IMIDAZOLES
LYSINE
MICE
MODIFICATIONS
MUTANTS
NITRIC OXIDE
PROTEINS
RESIDUES
TARGETS