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- W1981503268 abstract "Antagonists of the FimH adhesin, a protein almost universally present at the extremity of type-1 fimbriae expressed by Escherichia coli, have been abundantly in the spotlight as alternative treatments of urinary tract infections. The antagonists function as bacterial antiadhesives through highly specific α-d-mannose binding in a charged and polar pocket at the tip of the FimH lectin domain and by the stacking of alkyl or aromatic moieties substituted on the mannose with two tyrosine residues (Tyr48 and Tyr137) at the entrance of the mannose-binding pocket. Using high-resolution crystal data, interaction energies are calculated for the different observed aromatic stacking modes between the tyrosines and the antagonist. The dispersion component of the interaction energy correlates with the observed electron density. The quantum chemical reactivity descriptors local hardness and polarizability were successfully validated as prediction tools for ligand affinity in the tyrosine gate of FimH and therefore have potential for rapid drug screening." @default.
- W1981503268 created "2016-06-24" @default.
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- W1981503268 date "2013-09-18" @default.
- W1981503268 modified "2023-10-11" @default.
- W1981503268 title "Validation of Reactivity Descriptors to Assess the Aromatic Stacking within the Tyrosine Gate of FimH" @default.
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- W1981503268 doi "https://doi.org/10.1021/ml400269v" @default.
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