Target Mechanism-Based Whole-Cell Screening Identifies Bortezomib as an Inhibitor of Caseinolytic Protease in Mycobacteria

A novel type of antibacterial screening method, a target mechanism-based whole-cell screening method, was developed to combine the advantages of target mechanism- and whole-cell-based approaches. A mycobacterial reporter strain with a synthetic phenotype for caseinolytic protease (ClpP1P2) activity...

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Autores principales: Moreira, Wilfried, Ngan, Grace J. Y., Low, Jian Liang, Poulsen, Anders, Chia, Brian C. S., Ang, Melgious J. Y., Yap, Amelia, Fulwood, Justina, Lakshmanan, Umayal, Lim, Jolander, Khoo, Audrey Y. T., Flotow, Horst, Hill, Jeffrey, Raju, Ravikiran M., Rubin, Eric J., Dick, Thomas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society of Microbiology 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4436076/
https://www.ncbi.nlm.nih.gov/pubmed/25944857
http://dx.doi.org/10.1128/mBio.00253-15
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author Moreira, Wilfried
Ngan, Grace J. Y.
Low, Jian Liang
Poulsen, Anders
Chia, Brian C. S.
Ang, Melgious J. Y.
Yap, Amelia
Fulwood, Justina
Lakshmanan, Umayal
Lim, Jolander
Khoo, Audrey Y. T.
Flotow, Horst
Hill, Jeffrey
Raju, Ravikiran M.
Rubin, Eric J.
Dick, Thomas
author_facet Moreira, Wilfried
Ngan, Grace J. Y.
Low, Jian Liang
Poulsen, Anders
Chia, Brian C. S.
Ang, Melgious J. Y.
Yap, Amelia
Fulwood, Justina
Lakshmanan, Umayal
Lim, Jolander
Khoo, Audrey Y. T.
Flotow, Horst
Hill, Jeffrey
Raju, Ravikiran M.
Rubin, Eric J.
Dick, Thomas
author_sort Moreira, Wilfried
collection PubMed
description A novel type of antibacterial screening method, a target mechanism-based whole-cell screening method, was developed to combine the advantages of target mechanism- and whole-cell-based approaches. A mycobacterial reporter strain with a synthetic phenotype for caseinolytic protease (ClpP1P2) activity was engineered, allowing the detection of inhibitors of this enzyme inside intact bacilli. A high-throughput screening method identified bortezomib, a human 26S proteasome drug, as a potent inhibitor of ClpP1P2 activity and bacterial growth. A battery of secondary assays was employed to demonstrate that bortezomib indeed exerts its antimicrobial activity via inhibition of ClpP1P2: Down- or upmodulation of the intracellular protease level resulted in hyper- or hyposensitivity of the bacteria, the drug showed specific potentiation of translation error-inducing aminoglycosides, ClpP1P2-specific substrate WhiB1 accumulated upon exposure, and growth inhibition potencies of bortezomib derivatives correlated with ClpP1P2 inhibition potencies. Furthermore, molecular modeling showed that the drug can bind to the catalytic sites of ClpP1P2. This work demonstrates the feasibility of target mechanism-based whole-cell screening, provides chemical validation of ClpP1P2 as a target, and identifies a drug in clinical use as a new lead compound for tuberculosis therapy.
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spelling pubmed-44360762015-05-25 Target Mechanism-Based Whole-Cell Screening Identifies Bortezomib as an Inhibitor of Caseinolytic Protease in Mycobacteria Moreira, Wilfried Ngan, Grace J. Y. Low, Jian Liang Poulsen, Anders Chia, Brian C. S. Ang, Melgious J. Y. Yap, Amelia Fulwood, Justina Lakshmanan, Umayal Lim, Jolander Khoo, Audrey Y. T. Flotow, Horst Hill, Jeffrey Raju, Ravikiran M. Rubin, Eric J. Dick, Thomas mBio Research Article A novel type of antibacterial screening method, a target mechanism-based whole-cell screening method, was developed to combine the advantages of target mechanism- and whole-cell-based approaches. A mycobacterial reporter strain with a synthetic phenotype for caseinolytic protease (ClpP1P2) activity was engineered, allowing the detection of inhibitors of this enzyme inside intact bacilli. A high-throughput screening method identified bortezomib, a human 26S proteasome drug, as a potent inhibitor of ClpP1P2 activity and bacterial growth. A battery of secondary assays was employed to demonstrate that bortezomib indeed exerts its antimicrobial activity via inhibition of ClpP1P2: Down- or upmodulation of the intracellular protease level resulted in hyper- or hyposensitivity of the bacteria, the drug showed specific potentiation of translation error-inducing aminoglycosides, ClpP1P2-specific substrate WhiB1 accumulated upon exposure, and growth inhibition potencies of bortezomib derivatives correlated with ClpP1P2 inhibition potencies. Furthermore, molecular modeling showed that the drug can bind to the catalytic sites of ClpP1P2. This work demonstrates the feasibility of target mechanism-based whole-cell screening, provides chemical validation of ClpP1P2 as a target, and identifies a drug in clinical use as a new lead compound for tuberculosis therapy. American Society of Microbiology 2015-05-05 /pmc/articles/PMC4436076/ /pubmed/25944857 http://dx.doi.org/10.1128/mBio.00253-15 Text en Copyright © 2015 Moreira et al. http://creativecommons.org/licenses/by-nc-sa/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution-Noncommercial-ShareAlike 3.0 Unported license (http://creativecommons.org/licenses/by-nc-sa/3.0/) , which permits unrestricted noncommercial use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Moreira, Wilfried
Ngan, Grace J. Y.
Low, Jian Liang
Poulsen, Anders
Chia, Brian C. S.
Ang, Melgious J. Y.
Yap, Amelia
Fulwood, Justina
Lakshmanan, Umayal
Lim, Jolander
Khoo, Audrey Y. T.
Flotow, Horst
Hill, Jeffrey
Raju, Ravikiran M.
Rubin, Eric J.
Dick, Thomas
Target Mechanism-Based Whole-Cell Screening Identifies Bortezomib as an Inhibitor of Caseinolytic Protease in Mycobacteria
title Target Mechanism-Based Whole-Cell Screening Identifies Bortezomib as an Inhibitor of Caseinolytic Protease in Mycobacteria
title_full Target Mechanism-Based Whole-Cell Screening Identifies Bortezomib as an Inhibitor of Caseinolytic Protease in Mycobacteria
title_fullStr Target Mechanism-Based Whole-Cell Screening Identifies Bortezomib as an Inhibitor of Caseinolytic Protease in Mycobacteria
title_full_unstemmed Target Mechanism-Based Whole-Cell Screening Identifies Bortezomib as an Inhibitor of Caseinolytic Protease in Mycobacteria
title_short Target Mechanism-Based Whole-Cell Screening Identifies Bortezomib as an Inhibitor of Caseinolytic Protease in Mycobacteria
title_sort target mechanism-based whole-cell screening identifies bortezomib as an inhibitor of caseinolytic protease in mycobacteria
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4436076/
https://www.ncbi.nlm.nih.gov/pubmed/25944857
http://dx.doi.org/10.1128/mBio.00253-15
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