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Article Dans Une Revue Angewandte Chemie International Edition Année : 2016

A Three-Site Mechanism for Agonist/Antagonist Selective Binding to Vasopressin Receptors

Résumé

Molecular‐dynamics simulations with metadynamics enhanced sampling reveal three distinct binding sites for arginine vasopressin (AVP) within its V2‐receptor (V2R). Two of these, the vestibule and intermediate sites, block (antagonize) the receptor, and the third is the orthosteric activation (agonist) site. The contacts found for the orthosteric site satisfy all the requirements deduced from mutagenesis experiments. Metadynamics simulations for V2R and its V1aR‐analog give an excellent correlation with experimental binding free energies by assuming that the most stable binding site in the simulations corresponds to the experimental binding free energy in each case. The resulting three‐site mechanism separates agonists from antagonists and explains subtype selectivity

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https://hal.science/hal-02043755

Soumis le : jeudi 21 février 2019-11:11:17

Dernière modification le : jeudi 12 octobre 2023-11:48:05

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hal-02043755 , version 1 (21-02-2019)

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Noureldin Saleh, Giorgio Saladino, Francesco Gervasio, Elke Haensele, Lee Banting, et al.. A Three-Site Mechanism for Agonist/Antagonist Selective Binding to Vasopressin Receptors. Angewandte Chemie International Edition, 2016, 55 (28), pp.8008-8012. ⟨10.1002/ange.201602729⟩. ⟨hal-02043755⟩

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