Literature DB >> 22069333

E1-E2 interactions in ubiquitin and Nedd8 ligation pathways.

Zeynep Tokgöz1, Thomas J Siepmann, Frederick Streich, Brajesh Kumar, Jennifer M Klein, Arthur L Haas.   

Abstract

Initial rates of E1-catalyzed E2 transthiolation have been used as a reporter function to probe the mechanism of 125I-ubiquitin transfer between activation and ligation half-reactions of ubiquitin conjugation. A functional survey of 11 representative human E2 paralogs reveals similar Km for binding to human Uba1 ternary complex (Km(ave)=121±72 nm) and kcat for ubiquitin transfer (kcat(ave)=4.0±1.2 s(-1)), suggesting that they possess a conserved binding site and transition state geometry and that they compete for charging through differences in intracellular concentration. Sequence analysis and mutagenesis localize this binding motif to three basic residues within Helix 1 of the E2 core domain, confirmed by transthiolation kinetics. Partial conservation of the motif among E2 paralogs not recognized by Uba1 suggests that another factor(s) account for the absolute specificity of cognate E2 binding. Truncation of the Uba1 carboxyl-terminal β-grasp domain reduces cognate Ubc2b binding by 31-fold and kcat by 3.5×10(4)-fold, indicating contributions to E2 binding and transition state stabilization. Truncation of the paralogous domain from the Nedd8 activating enzyme has negligible effect on cognate Ubc12 transthiolation but abrogates E2 specificity toward non-cognate carrier proteins. Exchange of the β-grasp domains between ubiquitin and Nedd8 activating enzymes fails to reverse the effect of truncation. Thus, the conserved Helix 1 binding motif and the β-grasp domain direct general E2 binding, whereas the latter additionally serves as a specificity filter to exclude charging of non-cognate E2 paralogs in order to maintain the fidelity of downstream signaling.

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Year:  2011        PMID: 22069333      PMCID: PMC3249083          DOI: 10.1074/jbc.M111.294975

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  47 in total

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6.  Structure of an E6AP-UbcH7 complex: insights into ubiquitination by the E2-E3 enzyme cascade.

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3.  Convergent evolution in the assembly of polyubiquitin degradation signals by the Shigella flexneri IpaH9.8 ligase.

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Journal:  J Biol Chem       Date:  2014-10-23       Impact factor: 5.157

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5.  Tripartite motif ligases catalyze polyubiquitin chain formation through a cooperative allosteric mechanism.

Authors:  Frederick C Streich; Virginia P Ronchi; J Patrick Connick; Arthur L Haas
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6.  Structure of a ubiquitin E1-E2 complex: insights to E1-E2 thioester transfer.

Authors:  Shaun K Olsen; Christopher D Lima
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Review 7.  Structural and functional insights to ubiquitin-like protein conjugation.

Authors:  Frederick C Streich; Christopher D Lima
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8.  Crystal structure of a human ubiquitin E1-ubiquitin complex reveals conserved functional elements essential for activity.

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9.  Oligomerization of the HECT ubiquitin ligase NEDD4-2/NEDD4L is essential for polyubiquitin chain assembly.

Authors:  Dustin R Todaro; Allison C Augustus-Wallace; Jennifer M Klein; Arthur L Haas
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10.  Mechanistic study of Uba5 enzyme and the Ufm1 conjugation pathway.

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Journal:  J Biol Chem       Date:  2014-06-25       Impact factor: 5.157

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