Title of article
The Thioesterase Domain of the Fengycin Biosynthesis Cluster: A Structural Base for the Macrocyclization of a Non-ribosomal Lipopeptide
Author/Authors
Stefan A. Samel، نويسنده , , Bj?rn Wagner، نويسنده , , Mohamed A. Marahiel، نويسنده , , Lars-Oliver Essen، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2006
Pages
14
From page
876
To page
889
Abstract
Many secondary metabolic peptides from bacteria and fungi are produced by non-ribosomal peptide synthetases (NRPS) where the final step of biosynthesis is often catalysed by designated thioesterase domains. Here, we report the 1.8 Å crystal structure of the fengycin thioesterase (FenTE) from Bacillus subtilis F29-3, which catalyses the regio- and stereoselective release and macrocyclization of the antibiotic fengycin from the NRPS template. A structure of the PMSF-inactivated FenTE domain suggests the location of the oxyanion hole and the binding site of the C-terminal residue l-Ile11 of the lipopeptide. Using a combination of docking, molecular dynamics simulations and in vitro activity assays, a model of the FenTE–fengycin complex was derived in which peptide cyclization requires strategic interactions with residues lining the active site canyon.
Keywords
fengycin , non-ribosomal peptide synthesis , Macrocyclization , thioesterase structure , Catalytic triad
Journal title
Journal of Molecular Biology
Serial Year
2006
Journal title
Journal of Molecular Biology
Record number
1248033
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