Target Identification of Mycobacterium tuberculosis Phenotypic Hits Using a Concerted Chemogenomic, Biophysical, and Structural Approach

Mycobacterium phenotypic hits are a good reservoir for new chemotypes for the treatment of tuberculosis. However, the absence of defined molecular targets and modes of action could lead to failure in drug development. Therefore, a combination of ligand-based and structure-based chemogenomic approach...

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Autores principales: Mugumbate, Grace, Mendes, Vitor, Blaszczyk, Michal, Sabbah, Mohamad, Papadatos, George, Lelievre, Joel, Ballell, Lluis, Barros, David, Abell, Chris, Blundell, Tom L., Overington, John P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2017
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5623190/
https://www.ncbi.nlm.nih.gov/pubmed/29018348
http://dx.doi.org/10.3389/fphar.2017.00681
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author Mugumbate, Grace
Mendes, Vitor
Blaszczyk, Michal
Sabbah, Mohamad
Papadatos, George
Lelievre, Joel
Ballell, Lluis
Barros, David
Abell, Chris
Blundell, Tom L.
Overington, John P.
author_facet Mugumbate, Grace
Mendes, Vitor
Blaszczyk, Michal
Sabbah, Mohamad
Papadatos, George
Lelievre, Joel
Ballell, Lluis
Barros, David
Abell, Chris
Blundell, Tom L.
Overington, John P.
author_sort Mugumbate, Grace
collection PubMed
description Mycobacterium phenotypic hits are a good reservoir for new chemotypes for the treatment of tuberculosis. However, the absence of defined molecular targets and modes of action could lead to failure in drug development. Therefore, a combination of ligand-based and structure-based chemogenomic approaches followed by biophysical and biochemical validation have been used to identify targets for Mycobacterium tuberculosis phenotypic hits. Our approach identified EthR and InhA as targets for several hits, with some showing dual activity against these proteins. From the 35 predicted EthR inhibitors, eight exhibited an IC(50) below 50 μM against M. tuberculosis EthR and three were confirmed to be also simultaneously active against InhA. Further hit validation was performed using X-ray crystallography yielding eight new crystal structures of EthR inhibitors. Although the EthR inhibitors attain their activity against M. tuberculosis by hitting yet undefined targets, these results provide new lead compounds that could be further developed to be used to potentiate the effect of EthA activated pro-drugs, such as ethionamide, thus enhancing their bactericidal effect.
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spelling pubmed-56231902017-10-10 Target Identification of Mycobacterium tuberculosis Phenotypic Hits Using a Concerted Chemogenomic, Biophysical, and Structural Approach Mugumbate, Grace Mendes, Vitor Blaszczyk, Michal Sabbah, Mohamad Papadatos, George Lelievre, Joel Ballell, Lluis Barros, David Abell, Chris Blundell, Tom L. Overington, John P. Front Pharmacol Pharmacology Mycobacterium phenotypic hits are a good reservoir for new chemotypes for the treatment of tuberculosis. However, the absence of defined molecular targets and modes of action could lead to failure in drug development. Therefore, a combination of ligand-based and structure-based chemogenomic approaches followed by biophysical and biochemical validation have been used to identify targets for Mycobacterium tuberculosis phenotypic hits. Our approach identified EthR and InhA as targets for several hits, with some showing dual activity against these proteins. From the 35 predicted EthR inhibitors, eight exhibited an IC(50) below 50 μM against M. tuberculosis EthR and three were confirmed to be also simultaneously active against InhA. Further hit validation was performed using X-ray crystallography yielding eight new crystal structures of EthR inhibitors. Although the EthR inhibitors attain their activity against M. tuberculosis by hitting yet undefined targets, these results provide new lead compounds that could be further developed to be used to potentiate the effect of EthA activated pro-drugs, such as ethionamide, thus enhancing their bactericidal effect. Frontiers Media S.A. 2017-09-26 /pmc/articles/PMC5623190/ /pubmed/29018348 http://dx.doi.org/10.3389/fphar.2017.00681 Text en Copyright © 2017 Mugumbate, Mendes, Blaszczyk, Sabbah, Papadatos, Lelievre, Ballell, Barros, Abell, Blundell and Overington. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Mugumbate, Grace
Mendes, Vitor
Blaszczyk, Michal
Sabbah, Mohamad
Papadatos, George
Lelievre, Joel
Ballell, Lluis
Barros, David
Abell, Chris
Blundell, Tom L.
Overington, John P.
Target Identification of Mycobacterium tuberculosis Phenotypic Hits Using a Concerted Chemogenomic, Biophysical, and Structural Approach
title Target Identification of Mycobacterium tuberculosis Phenotypic Hits Using a Concerted Chemogenomic, Biophysical, and Structural Approach
title_full Target Identification of Mycobacterium tuberculosis Phenotypic Hits Using a Concerted Chemogenomic, Biophysical, and Structural Approach
title_fullStr Target Identification of Mycobacterium tuberculosis Phenotypic Hits Using a Concerted Chemogenomic, Biophysical, and Structural Approach
title_full_unstemmed Target Identification of Mycobacterium tuberculosis Phenotypic Hits Using a Concerted Chemogenomic, Biophysical, and Structural Approach
title_short Target Identification of Mycobacterium tuberculosis Phenotypic Hits Using a Concerted Chemogenomic, Biophysical, and Structural Approach
title_sort target identification of mycobacterium tuberculosis phenotypic hits using a concerted chemogenomic, biophysical, and structural approach
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5623190/
https://www.ncbi.nlm.nih.gov/pubmed/29018348
http://dx.doi.org/10.3389/fphar.2017.00681
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