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      The HtrA/DegP family protease MamE is a bifunctional protein with roles in magnetosome protein localization and magnetite biomineralization.

      Molecular Microbiology
      Amino Acid Sequence, Bacterial Proteins, genetics, metabolism, Ferrosoferric Oxide, Genes, Bacterial, Heat-Shock Proteins, Magnetics, Magnetosomes, enzymology, Magnetospirillum, Membrane Proteins, biosynthesis, Microscopy, Fluorescence, Mutagenesis, Site-Directed, Peptide Hydrolases, Periplasmic Proteins, Sequence Alignment, Serine Endopeptidases

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          Abstract

          Magnetotactic bacteria contain nanometre-sized, membrane-bound organelles, called magnetosomes, which are tasked with the biomineralization of small crystals of the iron oxide magnetite allowing the organism to use geomagnetic field lines for navigation. A key player in this process is the HtrA/DegP family protease MamE. In its absence, Magnetospirillum magneticum str AMB-1 is able to form magnetosome membranes but not magnetite crystals, a defect previously linked to the mislocalization of magnetosome proteins. In this work we use a directed genetic approach to find that MamE, and another predicted magnetosome-associated protease, MamO, likely function as proteases in vivo. However, as opposed to the complete loss of mamE where no biomineralization is observed, the protease-deficient variant of this protein still supports the initiation and formation of small, 20 nm-sized crystals of magnetite, too small to hold a permanent magnetic dipole moment. This analysis also reveals that MamE is a bifunctional protein with a protease-independent role in magnetosome protein localization and a protease-dependent role in maturation of small magnetite crystals. Together, these results imply the existence of a previously unrecognized 'checkpoint' in biomineralization where MamE moderates the completion of magnetite formation and thus committal to magneto-aerotaxis as the organism's dominant mode of navigating the environment. © 2011 Blackwell Publishing Ltd.

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