Literature DB >> 25010720

Nickel translocation between metallochaperones HypA and UreE in Helicobacter pylori.

Xinming Yang1, Hongyan Li, Tianfan Cheng, Wei Xia, Yau-Tsz Lai, Hongzhe Sun.   

Abstract

Incorporation of nickel ions to the active sites of urease and hydrogenase is prerequisite for the appropriate functions of the metalloenzymes. Such a process requires the participation of several accessory proteins. Interestingly, some of them are shared by the two enzymes in their maturation processes. In this work, we characterized the molecular details of the interaction of metallochaperones UreE and HypA in Helicobacter pylori. We show by chemical cross-linking and static light scattering that the UreE dimer binds to HypA to form a hetero-complex i.e. HypA-(UreE)2. The dissociation constant (Kd) of the protein complex was determined by ITC to be 1 μM in the absence of nickel ions; whereas binding of Ni(2+) but not Zn(2+) to UreE resulted in ca. one fold decrease in the affinity. The putative interfaces on HypA unveiled by NMR chemical shift perturbation were found mainly at the nickel binding domain and in the cleft between α1 and β1/β6. We also identified that the C-domain of UreE, in particular the C-terminal residues of 158-170 are indispensable for the interaction of UreE and HypA. Such an interaction was also observed intracellularly by GFP-fragment reassembly assay. Moreover, we demonstrated using a fluorescent probe that nickel is transferred from HypA to UreE via the specific protein-protein interaction. Deletion of the C-terminus (residues 158-170) of UreE abolished nickel transfer and led to a significant decrease in urease activity. This study provides direct in vitro and in vivo evidence as well as molecular details of nickel translocation mediated by protein-protein interaction.

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Year:  2014        PMID: 25010720     DOI: 10.1039/c4mt00134f

Source DB:  PubMed          Journal:  Metallomics        ISSN: 1756-5901            Impact factor:   4.526


  10 in total

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2.  The Helicobacter pylori HypA·UreE2 Complex Contains a Novel High-Affinity Ni(II)-Binding Site.

Authors:  Heidi Q Hu; Hsin-Ting Huang; Michael J Maroney
Journal:  Biochemistry       Date:  2018-05-10       Impact factor: 3.162

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4.  Structure and dynamics of Helicobacter pylori nickel-chaperone HypA: an integrated approach using NMR spectroscopy, functional assays and computational tools.

Authors:  Chris A E M Spronk; Szymon Żerko; Michał Górka; Wiktor Koźmiński; Benjamin Bardiaux; Barbara Zambelli; Francesco Musiani; Mario Piccioli; Priyanka Basak; Faith C Blum; Ryan C Johnson; Heidi Hu; D Scott Merrell; Michael Maroney; Stefano Ciurli
Journal:  J Biol Inorg Chem       Date:  2018-09-27       Impact factor: 3.358

5.  Structural insights into how GTP-dependent conformational changes in a metallochaperone UreG facilitate urease maturation.

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6.  UreE-UreG complex facilitates nickel transfer and preactivates GTPase of UreG in Helicobacter pylori.

Authors:  Xinming Yang; Hongyan Li; Tsz-Pui Lai; Hongzhe Sun
Journal:  J Biol Chem       Date:  2015-03-09       Impact factor: 5.157

7.  Dynamic HypA zinc site is essential for acid viability and proper urease maturation in Helicobacter pylori.

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Journal:  Metallomics       Date:  2015-04       Impact factor: 4.526

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Review 9.  Helicobacter pylori infection: An overview of bacterial virulence factors and pathogenesis.

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Review 10.  Flavodoxins as Novel Therapeutic Targets against Helicobacter pylori and Other Gastric Pathogens.

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  10 in total

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