Copper Binding Sites in the Manganese-Oxidizing Mnx Protein Complex Investigated by Electron Paramagnetic Resonance Spectroscopy

Lizhi Tao, Troy A. Stich, Shu Hao Liou, Alexandra V. Soldatova, David A. Delgadillo, Christine A. Romano, Thomas G. Spiro, David B. Goodin, Bradley M. Tebo, William H. Casey, R. David Britt

    Research output: Contribution to journalArticlepeer-review

    13 Scopus citations

    Abstract

    Manganese-oxide minerals (MnOx) are widely distributed over the Earth's surface, and their geochemical cycling is globally important. A multicopper oxidase (MCO) MnxG protein from marine Bacillus bacteria plays an essential role in producing MnOx minerals by oxidizing Mn2+(aq) at rates that are 3 to 5 orders of magnitude faster than abiotic rates. The MnxG protein is isolated as part of a multiprotein complex denoted as "Mnx" that includes accessory protein subunits MnxE and MnxF, with an estimated stoichiometry of MnxE3F3G and corresponding molecular weight of ?211 kDa. Herein, we report successful expression and isolation of the MCO MnxG protein without the E3F3 hexamer. This isolated MnxG shows activity for Mn2+(aq) oxidation to form manganese oxides. The complement of paramagnetic Cu(II) ions in the Mnx protein complex was examined by electron paramagnetic resonance (EPR) spectroscopy. Two distinct classes of type 2 Cu sites were detected. One class of Cu(II) site (denoted as T2Cu-A), located in the MnxG subunit, is identified by the magnetic parameters g? = 2.320 and A? = 510 MHz. The other class of Cu(II) sites (denoted as T2Cu-B) is characterized by g? = 2.210 and A? = 615 MHz and resides in the putative hexameric MnxE3F3 subunit. These different magnetic properties correlate with the differences in the reduction potentials of the respective Cu(II) centers. These studies provide new insights into the molecular mechanism of manganese biomineralization.

    Original languageEnglish (US)
    Pages (from-to)8868-8877
    Number of pages10
    JournalJournal of the American Chemical Society
    Volume139
    Issue number26
    DOIs
    StatePublished - Jul 5 2017

    ASJC Scopus subject areas

    • Catalysis
    • General Chemistry
    • Biochemistry
    • Colloid and Surface Chemistry

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