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Molecular basis of halorespiration control by CprK, a CRP-FNR type transcriptional regulator

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posted on 2016-04-22, 10:56 authored by C. Levy, K. Pike, D. J. Heyes, M. Gordon Joyce, K. Gabor, H. Smidt, J. van der Oost, D. Leys
Certain bacteria are able to conserve energy via the reductive dehalogenation of halo-organic compounds in a respiration-type metabolism. The transcriptional regulator CprK from Desulfitobacterium spp. induces expression of halorespiratory genes upon binding of o-chlorophenol ligands and is reversibly inactivated by oxygen through disulphide bond formation. We report crystal structures of D. hafniense CprK in the ligand-free (both oxidation states), ligand-bound (reduced) and DNA-bound states, making it the first member of the widespread CRP-FNR superfamily for which a complete structural description of both redox-dependent and allosteric molecular rearrangements is available. In conjunction with kinetic and thermodynamic ligand binding studies, we provide a model for the allosteric mechanisms underpinning transcriptional control. Amino acids that play a key role in this mechanism are not conserved in functionally distinct CRP-FNR members. This suggests that, despite significant structural homology, distinct allosteric mechanisms are used, enabling this protein family to control a very wide range of processes.

Funding

This work was supported by the BBSRC, D.L. is a Royal Society University Research Fellow.

History

Citation

Molecular Microbiology (2008) 70(1), 151–167

Version

  • VoR (Version of Record)

Published in

Molecular Microbiology (2008) 70(1)

Publisher

Wiley

issn

0950-382X

eissn

1365-2958

Acceptance date

2008-08-04

Copyright date

2008

Available date

2016-04-22

Publisher version

http://onlinelibrary.wiley.com/doi/10.1111/j.1365-2958.2008.06399.x/abstract

Language

en

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