The nisin–lipid II complex reveals a pyrophosphate cage that provides a blueprint for novel antibiotics

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作者
Shang-Te D Hsu
Eefjan Breukink
Eugene Tischenko
Mandy A G Lutters
Ben de Kruijff
Robert Kaptein
Alexandre M J J Bonvin
Nico A J van Nuland
机构
[1] Bijvoet Center for Biomolecular Research,Department of NMR Spectroscopy
[2] Utrecht University,Department of Biochemistry of Membranes
[3] Padualaan 8,undefined
[4] Bijvoet Center for Biomolecular Research,undefined
[5] Utrecht University,undefined
[6] Padualaan 8,undefined
来源
Nature Structural & Molecular Biology | 2004年 / 11卷
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摘要
The emerging antibiotics-resistance problem has underlined the urgent need for novel antimicrobial agents. Lantibiotics (lanthionine-containing antibiotics) are promising candidates to alleviate this problem. Nisin, a member of this family, has a unique pore-forming activity against bacteria. It binds to lipid II, the essential precursor of cell wall synthesis. As a result, the membrane permeabilization activity of nisin is increased by three orders of magnitude. Here we report the solution structure of the complex of nisin and lipid II. The structure shows a novel lipid II–binding motif in which the pyrophosphate moiety of lipid II is primarily coordinated by the N-terminal backbone amides of nisin via intermolecular hydrogen bonds. This cage structure provides a rationale for the conservation of the lanthionine rings among several lipid II–binding lantibiotics. The structure of the pyrophosphate cage offers a template for structure-based design of novel antibiotics.
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页码:963 / 967
页数:4
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