Literature DB >> 24548299

Structural and mechanistic insights into an extracytoplasmic copper trafficking pathway in Streptomyces lividans.

Katie L I M Blundell1, Michael A Hough1, Erik Vijgenboom2, Jonathan A R Worrall1.   

Abstract

In Streptomyces lividans an extracytoplasmic copper-binding Sco protein plays a role in two unlinked processes: (i) initiating a morphological development switch and (ii) facilitating the co-factoring of the CuA domain of CcO (cytochrome c oxidase). How Sco obtains copper once secreted to the extracytoplasmic environment is unknown. In the present paper we report on a protein possessing an HX₆MX₂₁HXM motif that binds a single cuprous ion with subfemtomolar affinity. High-resolution X-ray structures of this extracytoplasmic copper chaperone-like protein (ECuC) in the apo- and Cu(I)-bound states reveal that the latter possesses a surface-accessible cuprous-ion-binding site located in a dish-shaped region of β-sheet structure. A cuprous ion is transferred under a favourable thermodynamic gradient from ECuC to Sco with no back transfer occurring. The ionization properties of the cysteine residues in the Cys⁸⁶xxxCys⁹⁰ copper-binding motif of Sco, together with their positional locations identified from an X-ray structure of Sco, suggests a role for Cys⁸⁶ in initiating an inter-complex ligand-exchange reaction with Cu(I)-ECuC. Generation of the genetic knockouts, Δsco, Δecuc and Δsco/ecuc, and subsequent in vivo assays lend support to the existence of a branched extracytoplasmic copper-trafficking pathway in S. lividans. One branch requires both Sco and to a certain extent ECuC to cofactor the CuA domain, whereas the other uses only Sco to deliver copper to a cuproenzyme to initiate morphological development.

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Year:  2014        PMID: 24548299     DOI: 10.1042/BJ20140017

Source DB:  PubMed          Journal:  Biochem J        ISSN: 0264-6021            Impact factor:   3.857


  8 in total

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7.  Structural basis and mechanism for metallochaperone-assisted assembly of the CuA center in cytochrome oxidase.

Authors:  Fabia Canonica; Daniel Klose; Raphael Ledermann; Maximilian M Sauer; Helge K Abicht; Nick Quade; Alvar D Gossert; Serge Chesnov; Hans-Martin Fischer; Gunnar Jeschke; Hauke Hennecke; Rudi Glockshuber
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8.  The DyP-type peroxidase DtpA is a Tat-substrate required for GlxA maturation and morphogenesis in Streptomyces.

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  8 in total

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