Thiophenecarboxamide derivatives activated by EthA kill mycobacterium tuberculosis by inhibiting the CTP synthetase PyrG

Mori, Giorgia; Chiarelli, Laurent R.; Esposito, Marta; Makarov, Vadim; Bellinzoni, Marco; Hartkoorn, Ruben C.; Degiacomi, Giulia; Boldrin, Francesca; Ekins, Sean; Ribeiro, Ana Luisa de Jesus Lopes; Marino, Leonardo B. [UNESP]; Centárová, Ivana; Svetlíková, Zuzana; Blaško, Jaroslav; Kazakova, Elena; Lepioshkin, Alexander; Barilone, Nathalie; Zanoni, Giuseppe; Porta, Alessio; Fondi, Marco; Fani, Renato; Baulard, Alain R.; Mikušová, Katarína; Alzari, Pedro M.; Manganelli, Riccardo; Carvalho, Luiz Pedro S. de; Riccardi, Giovanna; Cole, Stewart T.; Pasca, Maria Rosalia

Publicação:
Thiophenecarboxamide derivatives activated by EthA kill mycobacterium tuberculosis by inhibiting the CTP synthetase PyrG

dc.contributor.author	Mori, Giorgia
dc.contributor.author	Chiarelli, Laurent R.
dc.contributor.author	Esposito, Marta
dc.contributor.author	Makarov, Vadim
dc.contributor.author	Bellinzoni, Marco
dc.contributor.author	Hartkoorn, Ruben C.
dc.contributor.author	Degiacomi, Giulia
dc.contributor.author	Boldrin, Francesca
dc.contributor.author	Ekins, Sean
dc.contributor.author	Ribeiro, Ana Luisa de Jesus Lopes
dc.contributor.author	Marino, Leonardo B. [UNESP]
dc.contributor.author	Centárová, Ivana
dc.contributor.author	Svetlíková, Zuzana
dc.contributor.author	Blaško, Jaroslav
dc.contributor.author	Kazakova, Elena
dc.contributor.author	Lepioshkin, Alexander
dc.contributor.author	Barilone, Nathalie
dc.contributor.author	Zanoni, Giuseppe
dc.contributor.author	Porta, Alessio
dc.contributor.author	Fondi, Marco
dc.contributor.author	Fani, Renato
dc.contributor.author	Baulard, Alain R.
dc.contributor.author	Mikušová, Katarína
dc.contributor.author	Alzari, Pedro M.
dc.contributor.author	Manganelli, Riccardo
dc.contributor.author	Carvalho, Luiz Pedro S. de
dc.contributor.author	Riccardi, Giovanna
dc.contributor.author	Cole, Stewart T.
dc.contributor.author	Pasca, Maria Rosalia
dc.contributor.institution	University of Pavia
dc.contributor.institution	Russian Academy of Science
dc.contributor.institution	Université Paris Diderot
dc.contributor.institution	Ecole Polytechnique Fédérale de Lausanne
dc.contributor.institution	University of Padova
dc.contributor.institution	Collaborative Drug Discovery
dc.contributor.institution	Francis Crick Institute
dc.contributor.institution	Universidade Estadual Paulista (Unesp)
dc.contributor.institution	Comenius University in Bratislava
dc.contributor.institution	University of Florence
dc.contributor.institution	Center for Infection and Immunity
dc.date.accessioned	2015-12-07T15:36:39Z
dc.date.available	2015-12-07T15:36:39Z
dc.date.issued	2015-07-23
dc.description.abstract	To combat the emergence of drug-resistant strains of Mycobacterium tuberculosis, new antitubercular agents and novel drug targets are needed. Phenotypic screening of a library of 594 hit compounds uncovered two leads that were active against M. tuberculosis in its replicating, non-replicating, and intracellular states: compounds 7947882 (5-methyl-N-(4-nitrophenyl)thiophene-2-carboxamide) and 7904688 (3-phenyl-N-[(4-piperidin-1-ylphenyl)carbamothioyl]propanamide). Mutants resistant to both compounds harbored mutations in ethA (rv3854c), the gene encoding the monooxygenase EthA, and/or in pyrG (rv1699) coding for the CTP synthetase, PyrG. Biochemical investigations demonstrated that EthA is responsible for the activation of the compounds, and by mass spectrometry we identified the active metabolite of 7947882, which directly inhibits PyrG activity. Metabolomic studies revealed that pharmacological inhibition of PyrG strongly perturbs DNA and RNA biosynthesis, and other metabolic processes requiring nucleotides. Finally, the crystal structure of PyrG was solved, paving the way for rational drug design with this newly validated drug target.	en
dc.description.affiliation	Department of Biology and Biotechnology Lazzaro Spallanzani, University of Pavia, Pavia, Italy
dc.description.affiliation	A. N. Bakh Institute of Biochemistry, Russian Academy of Science, Moscow, Russia
dc.description.affiliation	Institut Pasteur, Unité de Microbiologie Structurale, CNRS-UMR3528, Université Paris Diderot, Paris, France
dc.description.affiliation	Global Health Institute, Ecole Polytechnique Fédérale de Lausanne, Lausanne, Switzerland
dc.description.affiliation	Department of Molecular Medicine, University of Padova, Padua, Italy
dc.description.affiliation	Collaborative Drug Discovery, Bayshore Highway, Burlingame, CA, USA
dc.description.affiliation	Francis Crick Institute, Mill Hill Laboratory, The Ridgeway, Mill Hill, London, UK
dc.description.affiliation	Faculdade de Ciências Farmacêuticas (FCFAR), Universidade Estadual Paulista (UNESP), Araraquara, SP, Brasil
dc.description.affiliation	Department of Biochemistry, Faculty of Natural Sciences, Comenius University in Bratislava, Ilkovičova 6, Mlynská dolina, Bratislava, Slovakia
dc.description.affiliation	Institute of Chemistry, Faculty of Natural Sciences, Comenius University in Bratislava, Ilkovičova 6, Mlynská dolina, Bratislava, Slovak Republic
dc.description.affiliation	Department of Chemistry, University of Pavia, Pavia, Italy
dc.description.affiliation	Department of Biology, University of Florence, Sesto Fiorentino, Florence, Italy
dc.description.affiliation	Institut Pasteur de Lille, Center for Infection and Immunity, Lille, France
dc.description.affiliation	Francis Crick Institute, Mill Hill Laboratory, The Ridgeway, Mill Hill, London, UK
dc.description.affiliation	Global Health Institute, Ecole Polytechnique Fédérale de Lausanne, Lausanne, Switzerland
dc.description.affiliation	Department of Biology and Biotechnology Lazzaro Spallanzani, University of Pavia, Pavia, Italy
dc.description.affiliationUnesp	Faculdade de Ciências Farmacêuticas (FCFAR), Universidade Estadual Paulista (UNESP), Araraquara, SP, Brasil
dc.description.sponsorship	European Community’s Seventh Framework Program
dc.description.sponsorship	Slovak Research and Development Agency
dc.description.sponsorship	UK Medical Research Council
dc.description.sponsorship	Bill and Melinda Gates Foundation
dc.description.sponsorship	Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)
dc.description.sponsorship	Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq)
dc.description.sponsorship	Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)
dc.description.sponsorshipId	European Community’s Seventh Framework Program: 260872
dc.description.sponsorshipId	Slovak Research and Development Agency: DO7RP-0015-11
dc.description.sponsorshipId	UK Medical Research Council: MC_UP_A253_1111
dc.description.sponsorshipId	Bill and Melinda Gates Foundation: 49852
dc.description.sponsorshipId	FAPESP: 2011/21232-1
dc.description.sponsorshipId	CNPq: 140079/2013-0
dc.description.sponsorshipId	CAPES: 99999.003125/2014-09
dc.format.extent	917-927
dc.identifier	http://dx.doi.org/10.1016/j.chembiol.2015.05.016
dc.identifier.citation	Chemistry & Biology, v. 22, n. 7, p. 917-927, 2015.
dc.identifier.doi	10.1016/j.chembiol.2015.05.016
dc.identifier.issn	1879-1301
dc.identifier.pmc	PMC4521081
dc.identifier.pubmed	26097035
dc.identifier.uri	http://hdl.handle.net/11449/131507
dc.language.iso	eng
dc.publisher	Elsevier B. V.
dc.relation.ispartof	Chemistry & Biology
dc.rights.accessRights	Acesso restrito
dc.source	PubMed
dc.title	Thiophenecarboxamide derivatives activated by EthA kill mycobacterium tuberculosis by inhibiting the CTP synthetase PyrG	en
dc.type	Artigo
dcterms.rightsHolder	Elsevier B. V.
dspace.entity.type	Publication
unesp.campus	Universidade Estadual Paulista (UNESP), Faculdade de Ciências Farmacêuticas, Araraquara	pt
unesp.department	Análises Clínicas - FCF	pt

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Araraquara - FCF - Faculdade de Ciências Farmacêuticas

Publicação: Thiophenecarboxamide derivatives activated by EthA kill mycobacterium tuberculosis by inhibiting the CTP synthetase PyrG

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Publicação:
Thiophenecarboxamide derivatives activated by EthA kill mycobacterium tuberculosis by inhibiting the CTP synthetase PyrG