Literature DB >> 24097257

Archaeal ubiquitin-like SAMP3 is isopeptide-linked to proteins via a UbaA-dependent mechanism.

Hugo V Miranda1, Haike Antelmann, Nathaniel Hepowit, Nikita E Chavarria, David J Krause, Jonathan R Pritz, Katrin Bäsell, Dörte Becher, Matthew A Humbard, Luciano Brocchieri, Julie A Maupin-Furlow.   

Abstract

SAMP1 and SAMP2 are ubiquitin-like proteins that function as protein modifiers and are required for the production of sulfur-containing biomolecules in the archaeon Haloferax volcanii. Here we report a novel small archaeal modifier protein (named SAMP3) with a β-grasp fold and C-terminal diglycine motif characteristic of ubiquitin that is functional in protein conjugation in Hfx. volcanii. SAMP3 conjugates were dependent on the ubiquitin-activating E1 enzyme homolog of archaea (UbaA) for synthesis and were cleaved by the JAMM/MPN+ domain metalloprotease HvJAMM1. Twenty-three proteins (28 lysine residues) were found to be isopeptide-linked to the C-terminal carboxylate of SAMP3, and 331 proteins were reproducibly found associated with SAMP3 in a UbaA-dependent manner based on tandem mass spectrometry (MS/MS) analysis. The molybdopterin (MPT) synthase large subunit homolog MoaE, found samp3ylated at conserved active site lysine residues in MS/MS analysis, was also shown to be covalently bound to SAMP3 by immunoprecipitation and tandem affinity purifications. HvJAMM1 was demonstrated to catalyze the cleavage of SAMP3 from MoaE, suggesting a mechanism of controlling MPT synthase activity. The levels of samp3ylated proteins and samp3 transcripts were found to be increased by the addition of dimethyl sulfoxide to aerobically growing cells. Thus, we propose a model in which samp3ylation is covalent and reversible and controls the activity of enzymes such as MPT synthase. Sampylation of MPT synthase may govern the levels of molybdenum cofactor available and thus facilitate the scavenging of oxygen prior to the transition to respiration with molybdenum-cofactor-containing terminal reductases that use alternative electron acceptors such as dimethyl sulfoxide. Overall, our study of SAMP3 provides new insight into the diversity of functional ubiquitin-like protein modifiers and the network of ubiquitin-like protein targets in Archaea.

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Year:  2013        PMID: 24097257      PMCID: PMC3879616          DOI: 10.1074/mcp.M113.029652

Source DB:  PubMed          Journal:  Mol Cell Proteomics        ISSN: 1535-9476            Impact factor:   5.911


  65 in total

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Review 4.  Proteasomes and protein conjugation across domains of life.

Authors:  Julie Maupin-Furlow
Journal:  Nat Rev Microbiol       Date:  2011-12-19       Impact factor: 60.633

5.  Bioinformatic prediction and experimental verification of sRNAs in the haloarchaeon Haloferax volcanii.

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  19 in total

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2.  Rhodanese-Like Domain Protein UbaC and Its Role in Ubiquitin-Like Protein Modification and Sulfur Mobilization in Archaea.

Authors:  Nathaniel L Hepowit; Julie A Maupin-Furlow
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3.  Assays for ubiquitin-like protein ligation and proteasome function in archaea.

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Journal:  Methods Enzymol       Date:  2019-02-15       Impact factor: 1.600

Review 4.  Small Proteins in Archaea, a Mainly Unexplored World.

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Review 5.  Prokaryotic ubiquitin-like protein modification.

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Journal:  Annu Rev Microbiol       Date:  2014-05-29       Impact factor: 15.500

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Review 7.  Evolution of the archaeal and mammalian information processing systems: towards an archaeal model for human disease.

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10.  Proteome targets of ubiquitin-like samp1ylation are associated with sulfur metabolism and oxidative stress in Haloferax volcanii.

Authors:  Swathi Dantuluri; Yifei Wu; Nathaniel L Hepowit; Hui Chen; Sixue Chen; Julie A Maupin-Furlow
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