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PDBsum entry 4xoc
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Cell adhesion
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PDB id
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4xoc
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DOI no:
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Nat Commun
7:10738
(2016)
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PubMed id:
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Catch-bond mechanism of the bacterial adhesin FimH.
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M.M.Sauer,
R.P.Jakob,
J.Eras,
S.Baday,
D.Eriş,
G.Navarra,
S.Bernèche,
B.Ernst,
T.Maier,
R.Glockshuber.
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ABSTRACT
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Ligand-receptor interactions that are reinforced by mechanical stress, so-called
catch-bonds, play a major role in cell-cell adhesion. They critically contribute
to widespread urinary tract infections by pathogenic Escherichia coli strains.
These pathogens attach to host epithelia via the adhesin FimH, a two-domain
protein at the tip of type I pili recognizing terminal mannoses on epithelial
glycoproteins. Here we establish peptide-complemented FimH as a model system for
fimbrial FimH function. We reveal a three-state mechanism of FimH catch-bond
formation based on crystal structures of all states, kinetic analysis of ligand
interaction and molecular dynamics simulations. In the absence of tensile force,
the FimH pilin domain allosterically accelerates spontaneous ligand dissociation
from the FimH lectin domain by 100,000-fold, resulting in weak affinity.
Separation of the FimH domains under stress abolishes allosteric interplay and
increases the affinity of the lectin domain. Cell tracking demonstrates that
rapid ligand dissociation from FimH supports motility of piliated E. coli on
mannosylated surfaces in the absence of shear force.
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Links
