Probing the Allosteric Modulation of P-Glycoprotein: A Medicinal Chemistry Approach Toward the Identification of Noncompetitive P-Gp Inhibitors

[Image: see text] A medicinal chemistry approach combining in silico and in vitro methodologies was performed aiming at identifying and characterizing putative allosteric drug-binding sites (aDBSs) at the interface of the transmembrane- and nucleotide-binding domains (TMD-NBD) of P-glycoprotein. Two...

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Autores principales: Bonito, Cátia A., Ferreira, Ricardo J., Ferreira, Maria-José. U., Durães, Fernando, Sousa, Emília, Gillet, Jean-Pierre, Cordeiro, M. Natália D. S., dos Santos, Daniel J. V. A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2023
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10061618/
https://www.ncbi.nlm.nih.gov/pubmed/37008154
http://dx.doi.org/10.1021/acsomega.2c08273
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author Bonito, Cátia A.
Ferreira, Ricardo J.
Ferreira, Maria-José. U.
Durães, Fernando
Sousa, Emília
Gillet, Jean-Pierre
Cordeiro, M. Natália D. S.
dos Santos, Daniel J. V. A.
author_facet Bonito, Cátia A.
Ferreira, Ricardo J.
Ferreira, Maria-José. U.
Durães, Fernando
Sousa, Emília
Gillet, Jean-Pierre
Cordeiro, M. Natália D. S.
dos Santos, Daniel J. V. A.
author_sort Bonito, Cátia A.
collection PubMed
description [Image: see text] A medicinal chemistry approach combining in silico and in vitro methodologies was performed aiming at identifying and characterizing putative allosteric drug-binding sites (aDBSs) at the interface of the transmembrane- and nucleotide-binding domains (TMD-NBD) of P-glycoprotein. Two aDBSs were identified, one in TMD1/NBD1 and another one in TMD2/NBD2, by means of in silico fragment-based molecular dynamics and characterized in terms of size, polarity, and lining residues. From a small library of thioxanthone and flavanone derivatives, experimentally described to bind at the TMD-NBD interfaces, several compounds were identified to be able to decrease the verapamil-stimulated ATPase activity. An IC(50) of 81 ± 6.6 μM is reported for a flavanone derivative in the ATPase assays, providing evidence for an allosteric efflux modulation in P-glycoprotein. Molecular docking and molecular dynamics gave additional insights on the binding mode on how flavanone derivatives may act as allosteric inhibitors.
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spelling pubmed-100616182023-03-31 Probing the Allosteric Modulation of P-Glycoprotein: A Medicinal Chemistry Approach Toward the Identification of Noncompetitive P-Gp Inhibitors Bonito, Cátia A. Ferreira, Ricardo J. Ferreira, Maria-José. U. Durães, Fernando Sousa, Emília Gillet, Jean-Pierre Cordeiro, M. Natália D. S. dos Santos, Daniel J. V. A. ACS Omega [Image: see text] A medicinal chemistry approach combining in silico and in vitro methodologies was performed aiming at identifying and characterizing putative allosteric drug-binding sites (aDBSs) at the interface of the transmembrane- and nucleotide-binding domains (TMD-NBD) of P-glycoprotein. Two aDBSs were identified, one in TMD1/NBD1 and another one in TMD2/NBD2, by means of in silico fragment-based molecular dynamics and characterized in terms of size, polarity, and lining residues. From a small library of thioxanthone and flavanone derivatives, experimentally described to bind at the TMD-NBD interfaces, several compounds were identified to be able to decrease the verapamil-stimulated ATPase activity. An IC(50) of 81 ± 6.6 μM is reported for a flavanone derivative in the ATPase assays, providing evidence for an allosteric efflux modulation in P-glycoprotein. Molecular docking and molecular dynamics gave additional insights on the binding mode on how flavanone derivatives may act as allosteric inhibitors. American Chemical Society 2023-03-14 /pmc/articles/PMC10061618/ /pubmed/37008154 http://dx.doi.org/10.1021/acsomega.2c08273 Text en © 2023 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by/4.0/Permits the broadest form of re-use including for commercial purposes, provided that author attribution and integrity are maintained (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Bonito, Cátia A.
Ferreira, Ricardo J.
Ferreira, Maria-José. U.
Durães, Fernando
Sousa, Emília
Gillet, Jean-Pierre
Cordeiro, M. Natália D. S.
dos Santos, Daniel J. V. A.
Probing the Allosteric Modulation of P-Glycoprotein: A Medicinal Chemistry Approach Toward the Identification of Noncompetitive P-Gp Inhibitors
title Probing the Allosteric Modulation of P-Glycoprotein: A Medicinal Chemistry Approach Toward the Identification of Noncompetitive P-Gp Inhibitors
title_full Probing the Allosteric Modulation of P-Glycoprotein: A Medicinal Chemistry Approach Toward the Identification of Noncompetitive P-Gp Inhibitors
title_fullStr Probing the Allosteric Modulation of P-Glycoprotein: A Medicinal Chemistry Approach Toward the Identification of Noncompetitive P-Gp Inhibitors
title_full_unstemmed Probing the Allosteric Modulation of P-Glycoprotein: A Medicinal Chemistry Approach Toward the Identification of Noncompetitive P-Gp Inhibitors
title_short Probing the Allosteric Modulation of P-Glycoprotein: A Medicinal Chemistry Approach Toward the Identification of Noncompetitive P-Gp Inhibitors
title_sort probing the allosteric modulation of p-glycoprotein: a medicinal chemistry approach toward the identification of noncompetitive p-gp inhibitors
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10061618/
https://www.ncbi.nlm.nih.gov/pubmed/37008154
http://dx.doi.org/10.1021/acsomega.2c08273
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