Identification of Anti-Mycobacterium and Anti-Legionella Compounds With Potential Distinctive Structural Scaffolds From an HD-PBL Using Phenotypic Screens in Amoebae Host Models

Tubercular Mycobacteria and Legionella pneumophila are the causative agents of potentially fatal respiratory diseases due to their intrinsic pathogenesis but also due to the emergence of antibiotic resistance that limits treatment options. The aim of our study was to explore the antimicrobial activi...

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Autores principales: Hanna, Nabil, Kicka, Sébastien, Chiriano, Gianpaolo, Harrison, Christopher, Sakouhi, Hajer Ouertatani, Trofimov, Valentin, Kranjc, Agata, Nitschke, Jahn, Pagni, Marco, Cosson, Pierre, Hilbi, Hubert, Scapozza, Leonardo, Soldati, Thierry
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7047896/
https://www.ncbi.nlm.nih.gov/pubmed/32153546
http://dx.doi.org/10.3389/fmicb.2020.00266
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author Hanna, Nabil
Kicka, Sébastien
Chiriano, Gianpaolo
Harrison, Christopher
Sakouhi, Hajer Ouertatani
Trofimov, Valentin
Kranjc, Agata
Nitschke, Jahn
Pagni, Marco
Cosson, Pierre
Hilbi, Hubert
Scapozza, Leonardo
Soldati, Thierry
author_facet Hanna, Nabil
Kicka, Sébastien
Chiriano, Gianpaolo
Harrison, Christopher
Sakouhi, Hajer Ouertatani
Trofimov, Valentin
Kranjc, Agata
Nitschke, Jahn
Pagni, Marco
Cosson, Pierre
Hilbi, Hubert
Scapozza, Leonardo
Soldati, Thierry
author_sort Hanna, Nabil
collection PubMed
description Tubercular Mycobacteria and Legionella pneumophila are the causative agents of potentially fatal respiratory diseases due to their intrinsic pathogenesis but also due to the emergence of antibiotic resistance that limits treatment options. The aim of our study was to explore the antimicrobial activity of a small ligand-based chemical library of 1255 structurally diverse compounds. These compounds were screened in a combination of three assays, two monitoring the intracellular growth of the pathogenic bacteria, Mycobacterium marinum and L. pneumophila, and one assessing virulence of M. marinum. We set up these assays using two amoeba strains, the genetically tractable social amoeba Dictyostelium discoideum and the free-living amoeba Acanthamoeba castellanii. In summary, 64 (5.1%) compounds showed anti-infective/anti-virulence activity in at least one of the three assays. The intracellular assays hit rate varied between 1.7% (n = 22) for M. marinum and 2.8% (n = 35) for L. pneumophila with seven compounds in common for both pathogens. In parallel, 1.2% (n = 15) of the tested compounds were able to restore D. discoideum growth in the presence of M. marinum spiked in a lawn of food bacteria. We also validated the generality of the hits identified in the A. castellanii–M. marinum anti-infective screen using the D. discoideum–M. marinum host–pathogen model. The characterization of anti-infective and antibacterial hits in the latter infection model revealed compounds able to reduce intracellular growth more than 50% at 30 μM. Moreover, the chemical space and physico-chemical properties of the anti-M. marinum hits were compared to standard and candidate Mycobacterium tuberculosis (Mtb) drugs using ChemGPS-NP. A principle component analysis identified separate clusters for anti-M. marinum and anti-L. pneumophila hits unveiling the potentially new physico-chemical properties of these hits compared to standard and candidate M. tuberculosis drugs. Our studies underscore the relevance of using a combination of low-cost and low-complexity assays with full 3R compliance in concert with a rationalized focused library of compounds to identify new chemical scaffolds and to dissect some of their properties prior to taking further steps toward compound development.
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spelling pubmed-70478962020-03-09 Identification of Anti-Mycobacterium and Anti-Legionella Compounds With Potential Distinctive Structural Scaffolds From an HD-PBL Using Phenotypic Screens in Amoebae Host Models Hanna, Nabil Kicka, Sébastien Chiriano, Gianpaolo Harrison, Christopher Sakouhi, Hajer Ouertatani Trofimov, Valentin Kranjc, Agata Nitschke, Jahn Pagni, Marco Cosson, Pierre Hilbi, Hubert Scapozza, Leonardo Soldati, Thierry Front Microbiol Microbiology Tubercular Mycobacteria and Legionella pneumophila are the causative agents of potentially fatal respiratory diseases due to their intrinsic pathogenesis but also due to the emergence of antibiotic resistance that limits treatment options. The aim of our study was to explore the antimicrobial activity of a small ligand-based chemical library of 1255 structurally diverse compounds. These compounds were screened in a combination of three assays, two monitoring the intracellular growth of the pathogenic bacteria, Mycobacterium marinum and L. pneumophila, and one assessing virulence of M. marinum. We set up these assays using two amoeba strains, the genetically tractable social amoeba Dictyostelium discoideum and the free-living amoeba Acanthamoeba castellanii. In summary, 64 (5.1%) compounds showed anti-infective/anti-virulence activity in at least one of the three assays. The intracellular assays hit rate varied between 1.7% (n = 22) for M. marinum and 2.8% (n = 35) for L. pneumophila with seven compounds in common for both pathogens. In parallel, 1.2% (n = 15) of the tested compounds were able to restore D. discoideum growth in the presence of M. marinum spiked in a lawn of food bacteria. We also validated the generality of the hits identified in the A. castellanii–M. marinum anti-infective screen using the D. discoideum–M. marinum host–pathogen model. The characterization of anti-infective and antibacterial hits in the latter infection model revealed compounds able to reduce intracellular growth more than 50% at 30 μM. Moreover, the chemical space and physico-chemical properties of the anti-M. marinum hits were compared to standard and candidate Mycobacterium tuberculosis (Mtb) drugs using ChemGPS-NP. A principle component analysis identified separate clusters for anti-M. marinum and anti-L. pneumophila hits unveiling the potentially new physico-chemical properties of these hits compared to standard and candidate M. tuberculosis drugs. Our studies underscore the relevance of using a combination of low-cost and low-complexity assays with full 3R compliance in concert with a rationalized focused library of compounds to identify new chemical scaffolds and to dissect some of their properties prior to taking further steps toward compound development. Frontiers Media S.A. 2020-02-21 /pmc/articles/PMC7047896/ /pubmed/32153546 http://dx.doi.org/10.3389/fmicb.2020.00266 Text en Copyright © 2020 Hanna, Kicka, Chiriano, Harrison, Sakouhi, Trofimov, Kranjc, Nitschke, Pagni, Cosson, Hilbi, Scapozza and Soldati. 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) and the copyright owner(s) 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 Microbiology
Hanna, Nabil
Kicka, Sébastien
Chiriano, Gianpaolo
Harrison, Christopher
Sakouhi, Hajer Ouertatani
Trofimov, Valentin
Kranjc, Agata
Nitschke, Jahn
Pagni, Marco
Cosson, Pierre
Hilbi, Hubert
Scapozza, Leonardo
Soldati, Thierry
Identification of Anti-Mycobacterium and Anti-Legionella Compounds With Potential Distinctive Structural Scaffolds From an HD-PBL Using Phenotypic Screens in Amoebae Host Models
title Identification of Anti-Mycobacterium and Anti-Legionella Compounds With Potential Distinctive Structural Scaffolds From an HD-PBL Using Phenotypic Screens in Amoebae Host Models
title_full Identification of Anti-Mycobacterium and Anti-Legionella Compounds With Potential Distinctive Structural Scaffolds From an HD-PBL Using Phenotypic Screens in Amoebae Host Models
title_fullStr Identification of Anti-Mycobacterium and Anti-Legionella Compounds With Potential Distinctive Structural Scaffolds From an HD-PBL Using Phenotypic Screens in Amoebae Host Models
title_full_unstemmed Identification of Anti-Mycobacterium and Anti-Legionella Compounds With Potential Distinctive Structural Scaffolds From an HD-PBL Using Phenotypic Screens in Amoebae Host Models
title_short Identification of Anti-Mycobacterium and Anti-Legionella Compounds With Potential Distinctive Structural Scaffolds From an HD-PBL Using Phenotypic Screens in Amoebae Host Models
title_sort identification of anti-mycobacterium and anti-legionella compounds with potential distinctive structural scaffolds from an hd-pbl using phenotypic screens in amoebae host models
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7047896/
https://www.ncbi.nlm.nih.gov/pubmed/32153546
http://dx.doi.org/10.3389/fmicb.2020.00266
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