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Methanobactin and MmoD work in concert to act as the 'copper-switch' in methanotrophs.

Authors :
Semrau, Jeremy D.
Jagadevan, Sheeja
DiSpirito, Alan A.
Khalifa, Ashraf
Scanlan, Julie
Bergman, Brandt H.
Freemeier, Brittani C.
Baral, Bipin S.
Bandow, Nathan L.
Vorobev, Alexey
Haft, Daniel H.
Vuilleumier, Stéphane
Murrell, J. Colin
Source :
Environmental Microbiology; Nov2013, Vol. 15 Issue 11, p3077-3086, 10p
Publication Year :
2013

Abstract

Biological oxidation of methane to methanol by aerobic bacteria is catalysed by two different enzymes, the cytoplasmic or soluble methane monooxygenase ( sMMO) and the membrane-bound or particulate methane monooxygenase ( pMMO). Expression of MMOs is controlled by a 'copper-switch', i.e. sMMO is only expressed at very low copper : biomass ratios, while pMMO expression increases as this ratio increases. Methanotrophs synthesize a chalkophore, methanobactin, for the binding and import of copper. Previous work suggested that methanobactin was formed from a polypeptide precursor. Here we report that deletion of the gene suspected to encode for this precursor, mbnA, in Methylosinus trichosporium OB3b, abolishes methanobactin production. Further, gene expression assays indicate that methanobactin, together with another polypeptide of previously unknown function, MmoD, play key roles in regulating expression of MMOs. Based on these data, we propose a general model explaining how expression of the MMO operons is regulated by copper, methanobactin and MmoD. The basis of the 'copper-switch' is MmoD, and methanobactin amplifies the magnitude of the switch. Bioinformatic analysis of bacterial genomes indicates that the production of methanobactin-like compounds is not confined to methanotrophs, suggesting that its use as a metal-binding agent and/or role in gene regulation may be widespread in nature. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
14622912
Volume :
15
Issue :
11
Database :
Complementary Index
Journal :
Environmental Microbiology
Publication Type :
Academic Journal
Accession number :
92902075
Full Text :
https://doi.org/10.1111/1462-2920.12150