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Structural and thermodynamic characterization of the adrenodoxin-like domain of the electron-transfer protein Etp1 from Schizosaccharomyces pombe
Authors:Müller Jürgen J  Hannemann Frank  Schiffler Burkhard  Ewen Kerstin M  Kappl Reinhard  Heinemann Udo  Bernhardt Rita
Affiliation:
  • a Max-Delbrück-Centrum für Molekulare Medizin, Berlin, Germany
  • b FR 8.3 - Biochemie, Universität des Saarlandes, Saarbrücken, Germany
  • c FR 2.5 - Biophysik, Universität des Saarlandes, Saarbrücken, Germany
  • d Institut für Chemie und Biochemie, Freie Universität, Berlin, Germany
  • Abstract:The protein Etp1 of Schizosaccharomyces pombe consists of an amino-terminal COX15-like domain and a carboxy-terminal ferredoxin-like domain, Etp1fd, which is cleaved off after mitochondrial import. The physiological function of Etp1fd is supposed to lie in the participation in the assembly of iron-sulfur clusters and the synthesis of heme A. In addition, the protein was shown to be the first microbial ferredoxin being able to support electron transfer in mitochondrial steroid hydroxylating cytochrome P450 systems in vivo and in vitro, replacing thereby the native redox partner, adrenodoxin. Despite a sequence similarity of 39% and the fact that fission yeast is a mesophilic organism, thermodynamic studies revealed that Etp1fd has a melting temperature more than 20 °C higher than adrenodoxin. The three-dimensional structure of Etp1fd has been determined by crystallography. To the best of our knowledge it represents the first three-dimensional structure of a yeast ferredoxin. The structure-based sequence alignment of Etp1fd with adrenodoxin yields a rational explanation for their observed mutual exchangeability in the cytochrome P450 system. Analysis of the electron exchange with the S. pombe redox partner Arh1 revealed differences between Etp1fd and adrenodoxin, which might be linked to their different physiological functions in the mitochondria of mammals and yeast.
    Keywords:Crystal structure   Electron transfer   Iron-sulfur protein   Protein folding   Iron-sulfur-cluster synthesis   Ferredoxin
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