Archives of Microbiology

, Volume 194, Issue 3, pp 157–166 | Cite as

Crystal structure of the complex between 4-hydroxybutyrate CoA-transferase from Clostridium aminobutyricum and CoA

  • Sofia Macieira
  • Jin Zhang
  • Wolfgang Buckel
  • Albrecht Messerschmidt
Original Paper
First Online:
Received:
Revised:
Accepted:

Abstract

Clostridium aminobutyricum ferments 4-aminobutyrate (γ-aminobutyrate, GABA) to ammonia, acetate and butyrate via 4-hydroxybutyrate that is activated to the CoA-thioester catalyzed by 4-hydroxybutyrate CoA-transferase. Then, 4-hydroxybutyryl-CoA is dehydrated to crotonyl-CoA, which disproportionates to butyryl-CoA and acetyl-CoA. Cocrystallization of the CoA-transferase with the alternate substrate butyryl-CoA yielded crystals with non-covalently bound CoA and two water molecules at the active site. Most likely, butyryl-CoA reacted with the active site Glu238 to CoA and the mixed anhydride, which slowly hydrolyzed during crystallization. The structure of the CoA is similar but less stretched than that of the CoA-moiety of the covalent enzyme-CoA-thioester in 4-hydroxybutyrate CoA-transferase from Shewanella oneidensis. In contrast to the structures of the apo-enzyme and enzyme-CoA-thioester, the structure described here has a closed conformation, probably caused by a flip of the active site loop (residues 215–219). During turnover, the closed conformation may protect the anhydride intermediate from hydrolysis and CoA from dissociation from the enzyme. Hence, one catalytic cycle changes conformation of the enzyme four times: free enzyme—open conformation, CoA+ anhydride 1—closed, enzyme-CoA-thioester—open, CoA + anhydride-2—closed, free enzyme—open.

Keywords

Coenzyme A Crystal structure Enzyme complex 
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Notes

Acknowledgments

This work was supported by the European Commission (Contract no. 031220, “Spine2-complexes”). The production and analysis of the enzyme were supported by funds from the German Research Foundation (DFG), Fonds der Chemischen Industrie and the Max-Planck-Society. We thank Prof. Matthias Mann for his continuous interest in the project and valuable discussion and Dr. Grzegorz Popowicz for doing the data collection at the SLS in Villigen, Switzerland.

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Copyright information

© Springer-Verlag 2011

Authors and Affiliations

  • Sofia Macieira
    • 1
  • Jin Zhang
    • 2
  • Wolfgang Buckel
    • 2
    • 3
  • Albrecht Messerschmidt
    • 1
  1. 1.Department of Proteomics and Signal TransductionMax-Planck Institute of BiochemistryMartinsriedGermany
  2. 2.Laboratory for Microbiology, Department of BiologyPhilipps UniversitätMarburgGermany
  3. 3.Max-Planck Institute of Terrestrial MicrobiologyMarburgGermany

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