Literature DB >> 22045417

Multifaceted SlyD from Helicobacter pylori: implication in [NiFe] hydrogenase maturation.

Tianfan Cheng1, Hongyan Li, Wei Xia, Hongzhe Sun.   

Abstract

SlyD belongs to the FK506-binding protein (FKBP) family with both peptidylprolyl isomerase (PPIase) and chaperone activities, and is considered to be a ubiquitous cytosolic protein-folding facilitator in bacteria. It possesses a histidine- and cysteine-rich C-terminus binding to selected divalent metal ions (e.g., Ni(2+), Zn(2+)), which is important for its involvement in the maturation processes of metalloenzymes. We have determined the solution structure of C-terminus-truncated SlyD from Helicobacter pylori (HpSlyDΔC). HpSlyDΔC folds into two well-separated, orientation-independent domains: the PPIase-active FKBP domain and the chaperone-active insert-in-flap (IF) domain. The FKBP domain consists of a four-stranded antiparallel β-sheet with an α-helix on one side, whereas the IF domain folds into a four-stranded antiparallel β-sheet accompanied by a short α-helix. Intact H. pylori SlyD binds both Ni(2+) and Zn(2+), with dissociation constants of 2.74 and 3.79 μM respectively. Intriguingly, binding of Ni(2+) instead of Zn(2+) induces protein conformational changes around the active sites of the FKBP domain, implicating a regulatory role of nickel. The twin-arginine translocation (Tat) signal peptide from the small subunit of [NiFe] hydrogenase (HydA) binds the protein at the IF domain. Nickel binding and the recognition of the Tat signal peptide by the protein suggest that SlyD participates in [NiFe] hydrogenase maturation processes.

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Year:  2011        PMID: 22045417      PMCID: PMC3292732          DOI: 10.1007/s00775-011-0855-y

Source DB:  PubMed          Journal:  J Biol Inorg Chem        ISSN: 0949-8257            Impact factor:   3.358


  51 in total

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Review 4.  Specific metal recognition in nickel trafficking.

Authors:  Khadine A Higgins; Carolyn E Carr; Michael J Maroney
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6.  Metallochaperone UreG serves as a new target for design of urease inhibitor: A novel strategy for development of antimicrobials.

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7.  HpSlyD inducing CDX2 and VIL1 expression mediated through TCTP protein may contribute to intestinal metaplasia in the stomach.

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