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Details

Autor(en) / Beteiligte
Titel
Three-Dimensional Structure in Lipid Micelles of the Pediocin-like Antimicrobial Peptide Sakacin P and a Sakacin P Variant That Is Structurally Stabilized by an Inserted C-Terminal Disulfide Bridge
Ist Teil von
  • Biochemistry (Easton), 2003-10, Vol.42 (39), p.11417-11426
Ort / Verlag
United States: American Chemical Society
Erscheinungsjahr
2003
Quelle
MEDLINE
Beschreibungen/Notizen
  • The three-dimensional structures in dodecylphosphocholine (DPC) micelles and in trifluoroethanol (TFE) of the pediocin-like antimicrobial peptide sakacin P and an engineered variant of sakacin P (termed sakP[N24C+44C]) have been determined by use of nuclear magnetic resonance spectroscopy. SakP[N24C+44C] has an inserted non-native activity- and structure-stabilizing C-terminal disulfide bridge that ties the C-terminus to the middle part of the peptide. In the presence of DPC, the cationic N-terminal region (residues 1−17) of both peptides has an S-shaped conformation that is reminiscent of a three-stranded antiparallel β-sheet and that is more pronounced when the peptide was dissolved in TFE instead of DPC. The four positively charged residues located in the N-terminal part are found pointing to the same direction. For both peptides, the N-terminal region is followed by a well-defined central amphiphilic α-helix (residues 18−33), and this in turn is followed by the C-terminal tail (residues 34−43 for sakacin P and 34−44 for sakP[N24C+44C]) that lacks any apparent common secondary structural motif. In the presence of DPC, the C-terminal tails in both peptides fold back onto the central α-helix, thereby creating a hairpin-like structure in the C-terminal halves. The lack of long-range NOEs between the β-sheet Ν-terminal region and the hairpin-like C-terminal half indicates that there is a flexible hinge between these regions. We discuss which implications such a structural arrangement has on the interaction with the target cell membrane.

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