A multitarget approach to drug discovery inhibiting Mycobacterium tuberculosis PyrG and PanK

Laurent R. Chiarelli; Giorgia Mori; Beatrice Silvia Orena; Marta Esposito; Thomas Lane; Ana Luisa De Jesus Lopes Ribeiro; Giulia Degiacomi; Júlia Zemanová; Sára Szádocka; Stanislav Huszár; Zuzana Palčeková; Marcello Manfredi; Fabio Gosetti; Joël Lelièvre; Lluis Ballell; Elena Kazakova; Vadim Makarov; Emilio Marengo; Katarina Mikusova; Stewart T. Cole; Giovanna Riccardi; Sean Ekins; Maria Rosalia Pasca

doi:10.1038/s41598-018-21614-4

A multitarget approach to drug discovery inhibiting Mycobacterium tuberculosis PyrG and PanK

Laurent R. Chiarelli
, Giorgia Mori
, Beatrice Silvia Orena
, Marta Esposito
, Thomas Lane
, Ana Luisa De Jesus Lopes Ribeiro
, Giulia Degiacomi
, Júlia Zemanová
, Sára Szádocka
, Stanislav Huszár
, Zuzana Palčeková
, Marcello Manfredi
, Fabio Gosetti
, Joël Lelièvre
, Lluis Ballell
, Elena Kazakova
, Vadim Makarov
, Emilio Marengo
, Katarina Mikusova
, Stewart T. Cole

Giovanna Riccardi, Sean Ekins, Maria Rosalia Pasca

Risultato della ricerca: Contributo su rivista › Articolo in rivista › peer review

Abstract

Mycobacterium tuberculosis, the etiological agent of the infectious disease tuberculosis, kills approximately 1.5 million people annually, while the spread of multidrug-resistant strains is of great global concern. Thus, continuous efforts to identify new antitubercular drugs as well as novel targets are crucial. Recently, two prodrugs activated by the monooxygenase EthA, 7947882 and 7904688, which target the CTP synthetase PyrG, were identified and characterized. In this work, microbiological, biochemical, and in silico methodologies were used to demonstrate that both prodrugs possess a second target, the pantothenate kinase PanK. This enzyme is involved in coenzyme A biosynthesis, an essential pathway for M. tuberculosis growth. Moreover, compound 11426026, the active metabolite of 7947882, was demonstrated to directly inhibit PanK, as well. In an independent screen of a compound library against PyrG, two additional inhibitors were also found to be active against PanK. In conclusion, these direct PyrG and PanK inhibitors can be considered as leads for multitarget antitubercular drugs and these two enzymes could be employed as a "double-tool" in order to find additional hit compounds.

Lingua originale	Inglese
Numero di articolo	3187
Rivista	Scientific Reports
Volume	8
Numero di pubblicazione	1
DOI	https://doi.org/10.1038/s41598-018-21614-4
Stato di pubblicazione	Pubblicato - 1 dic 2018

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Chiarelli, L. R., Mori, G., Orena, B. S., Esposito, M., Lane, T., De Jesus Lopes Ribeiro, A. L., Degiacomi, G., Zemanová, J., Szádocka, S., Huszár, S., Palčeková, Z., Manfredi, M., Gosetti, F., Lelièvre, J., Ballell, L., Kazakova, E., Makarov, V., Marengo, E., Mikusova, K., ... Pasca, M. R. (2018). A multitarget approach to drug discovery inhibiting Mycobacterium tuberculosis PyrG and PanK. Scientific Reports, 8(1), Articolo 3187. https://doi.org/10.1038/s41598-018-21614-4

@article{6f324e189d284e0594699a77b5775ff3,

title = "A multitarget approach to drug discovery inhibiting Mycobacterium tuberculosis PyrG and PanK",

abstract = "Mycobacterium tuberculosis, the etiological agent of the infectious disease tuberculosis, kills approximately 1.5 million people annually, while the spread of multidrug-resistant strains is of great global concern. Thus, continuous efforts to identify new antitubercular drugs as well as novel targets are crucial. Recently, two prodrugs activated by the monooxygenase EthA, 7947882 and 7904688, which target the CTP synthetase PyrG, were identified and characterized. In this work, microbiological, biochemical, and in silico methodologies were used to demonstrate that both prodrugs possess a second target, the pantothenate kinase PanK. This enzyme is involved in coenzyme A biosynthesis, an essential pathway for M. tuberculosis growth. Moreover, compound 11426026, the active metabolite of 7947882, was demonstrated to directly inhibit PanK, as well. In an independent screen of a compound library against PyrG, two additional inhibitors were also found to be active against PanK. In conclusion, these direct PyrG and PanK inhibitors can be considered as leads for multitarget antitubercular drugs and these two enzymes could be employed as a {"}double-tool{"} in order to find additional hit compounds.",

author = "Chiarelli, \{Laurent R.\} and Giorgia Mori and Orena, \{Beatrice Silvia\} and Marta Esposito and Thomas Lane and \{De Jesus Lopes Ribeiro\}, \{Ana Luisa\} and Giulia Degiacomi and J{\'u}lia Zemanov{\'a} and S{\'a}ra Sz{\'a}docka and Stanislav Husz{\'a}r and Zuzana Pal{\v c}ekov{\'a} and Marcello Manfredi and Fabio Gosetti and Jo{\"e}l Leli{\`e}vre and Lluis Ballell and Elena Kazakova and Vadim Makarov and Emilio Marengo and Katarina Mikusova and Cole, \{Stewart T.\} and Giovanna Riccardi and Sean Ekins and Pasca, \{Maria Rosalia\}",

note = "Publisher Copyright: {\textcopyright} 2018 The Author(s).",

year = "2018",

month = dec,

day = "1",

doi = "10.1038/s41598-018-21614-4",

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Chiarelli, LR, Mori, G, Orena, BS, Esposito, M, Lane, T, De Jesus Lopes Ribeiro, AL, Degiacomi, G, Zemanová, J, Szádocka, S, Huszár, S, Palčeková, Z, Manfredi, M, Gosetti, F, Lelièvre, J, Ballell, L, Kazakova, E, Makarov, V, Marengo, E, Mikusova, K, Cole, ST, Riccardi, G, Ekins, S & Pasca, MR 2018, 'A multitarget approach to drug discovery inhibiting Mycobacterium tuberculosis PyrG and PanK', Scientific Reports, vol. 8, n. 1, 3187. https://doi.org/10.1038/s41598-018-21614-4

TY - JOUR

T1 - A multitarget approach to drug discovery inhibiting Mycobacterium tuberculosis PyrG and PanK

AU - Chiarelli, Laurent R.

AU - Mori, Giorgia

AU - Orena, Beatrice Silvia

AU - Esposito, Marta

AU - Lane, Thomas

AU - De Jesus Lopes Ribeiro, Ana Luisa

AU - Degiacomi, Giulia

AU - Zemanová, Júlia

AU - Szádocka, Sára

AU - Huszár, Stanislav

AU - Palčeková, Zuzana

AU - Manfredi, Marcello

AU - Gosetti, Fabio

AU - Lelièvre, Joël

AU - Ballell, Lluis

AU - Kazakova, Elena

AU - Makarov, Vadim

AU - Marengo, Emilio

AU - Mikusova, Katarina

AU - Cole, Stewart T.

AU - Riccardi, Giovanna

AU - Ekins, Sean

AU - Pasca, Maria Rosalia

PY - 2018/12/1

Y1 - 2018/12/1

N2 - Mycobacterium tuberculosis, the etiological agent of the infectious disease tuberculosis, kills approximately 1.5 million people annually, while the spread of multidrug-resistant strains is of great global concern. Thus, continuous efforts to identify new antitubercular drugs as well as novel targets are crucial. Recently, two prodrugs activated by the monooxygenase EthA, 7947882 and 7904688, which target the CTP synthetase PyrG, were identified and characterized. In this work, microbiological, biochemical, and in silico methodologies were used to demonstrate that both prodrugs possess a second target, the pantothenate kinase PanK. This enzyme is involved in coenzyme A biosynthesis, an essential pathway for M. tuberculosis growth. Moreover, compound 11426026, the active metabolite of 7947882, was demonstrated to directly inhibit PanK, as well. In an independent screen of a compound library against PyrG, two additional inhibitors were also found to be active against PanK. In conclusion, these direct PyrG and PanK inhibitors can be considered as leads for multitarget antitubercular drugs and these two enzymes could be employed as a "double-tool" in order to find additional hit compounds.

AB - Mycobacterium tuberculosis, the etiological agent of the infectious disease tuberculosis, kills approximately 1.5 million people annually, while the spread of multidrug-resistant strains is of great global concern. Thus, continuous efforts to identify new antitubercular drugs as well as novel targets are crucial. Recently, two prodrugs activated by the monooxygenase EthA, 7947882 and 7904688, which target the CTP synthetase PyrG, were identified and characterized. In this work, microbiological, biochemical, and in silico methodologies were used to demonstrate that both prodrugs possess a second target, the pantothenate kinase PanK. This enzyme is involved in coenzyme A biosynthesis, an essential pathway for M. tuberculosis growth. Moreover, compound 11426026, the active metabolite of 7947882, was demonstrated to directly inhibit PanK, as well. In an independent screen of a compound library against PyrG, two additional inhibitors were also found to be active against PanK. In conclusion, these direct PyrG and PanK inhibitors can be considered as leads for multitarget antitubercular drugs and these two enzymes could be employed as a "double-tool" in order to find additional hit compounds.

UR - https://www.scopus.com/pages/publications/85042225158

U2 - 10.1038/s41598-018-21614-4

DO - 10.1038/s41598-018-21614-4

M3 - Article

SN - 2045-2322

VL - 8

JO - Scientific Reports

JF - Scientific Reports

IS - 1

M1 - 3187

ER -

A multitarget approach to drug discovery inhibiting Mycobacterium tuberculosis PyrG and PanK

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