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Journal article

Single-molecule interrogation of a bacterial sugar transporter allows the discovery of an extracellular inhibitor.

Abstract:
Capsular polysaccharides form the outermost protective layer around many Gram-negative bacteria. Antibiotics aimed directly at weakening this layer are not yet available. In pathogenic Escherichia coli E69, a protein, Wza, forms a pore in the outer membrane that transports K30 capsular polysaccharide from its site of synthesis to the outside of the cell. This therefore represents a prospective antibiotic target. Here we test a variety of grommet-like mimics of K30 capsular polysaccharide on wild-type Wza and on mutant open forms of the pore by electrical recording in planar lipid bilayers. The most effective glycomimetic was the unnatural cyclic octasaccharide octakis(6-deoxy-6-amino)cyclomaltooctaose (am8γCD), which blocks the α-helix barrel of Wza, a site that is directly accessible from the external medium. This glycomimetic inhibited K30 polysaccharide transport in live E. coli E69. With the protective outer membrane disrupted, the bacteria can be recognized and killed by the human immune system.
Publication status:
Published

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Publisher copy:
10.1038/nchem.1695

Authors

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Institution:
University of Oxford
Division:
MPLS
Department:
Chemistry
Sub department:
Organic Chemistry
Role:
Author


Journal:
Nature chemistry More from this journal
Volume:
5
Issue:
8
Pages:
651-659
Publication date:
2013-08-01
DOI:
EISSN:
1755-4349
ISSN:
1755-4330


Language:
English
Keywords:
Pubs id:
pubs:414462
UUID:
uuid:1a35de15-772f-4efb-a762-e5a762e45eef
Local pid:
pubs:414462
Source identifiers:
414462
Deposit date:
2013-11-17
ARK identifier:

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