| Literature DB >> 20508130 |
Tanja Schneider1, Thomas Kruse, Reinhard Wimmer, Imke Wiedemann, Vera Sass, Ulrike Pag, Andrea Jansen, Allan K Nielsen, Per H Mygind, Dorotea S Raventós, Søren Neve, Birthe Ravn, Alexandre M J J Bonvin, Leonardo De Maria, Anders S Andersen, Lora K Gammelgaard, Hans-Georg Sahl, Hans-Henrik Kristensen.
Abstract
Host defense peptides such as defensins are components of innate immunity and have retained antibiotic activity throughout evolution. Their activity is thought to be due to amphipathic structures, which enable binding and disruption of microbial cytoplasmic membranes. Contrary to this, we show that plectasin, a fungal defensin, acts by directly binding the bacterial cell-wall precursor Lipid II. A wide range of genetic and biochemical approaches identify cell-wall biosynthesis as the pathway targeted by plectasin. In vitro assays for cell-wall synthesis identified Lipid II as the specific cellular target. Consistently, binding studies confirmed the formation of an equimolar stoichiometric complex between Lipid II and plectasin. Furthermore, key residues in plectasin involved in complex formation were identified using nuclear magnetic resonance spectroscopy and computational modeling.Entities:
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Year: 2010 PMID: 20508130 DOI: 10.1126/science.1185723
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728