Your search keyword '"Villela AD"' showing total 26 results

1. Anti-tubercular profile of new selenium-menadione conjugates against Mycobacterium tuberculosis H37Rv (ATCC 27294) strain and multidrug-resistant clinical isolates.

Author

Ribeiro RCB, de Marins DB, Di Leo I, da Silva Gomes L, de Moraes MG, Abbadi BL, Villela AD, da Silva WF, da Silva LCRP, Machado P, Bizarro CV, Basso LA, Cristina de Moraes M, Ferreira VF, da Silva FC, and Nascimento V

Subjects

Animals, Antitubercular Agents chemical synthesis, Antitubercular Agents chemistry, Chlorocebus aethiops, Humans, Models, Molecular, Selenium chemistry, Tuberculosis drug therapy, Vero Cells, Vitamin K 3 analogs & derivatives, Vitamin K 3 chemical synthesis, Antitubercular Agents pharmacology, Mycobacterium tuberculosis drug effects, Selenium pharmacology, Vitamin K 3 pharmacology

Abstract

Tuberculosis (TB) is one of the most fatal diseases and is responsible for the infection of millions of people around the world. Most recently, scientific frontiers have been engaged to develop new drugs that can overcome drug-resistant TB. Following this direction, using a designed scaffold based on the combination of two separate pharmacophoric groups, a series of menadione-derived selenoesters was developed with good yields. All products were evaluated for their in vitro activity against Mycobacterium tuberculosis H37Rv and attractive results were observed, especially for the compounds 8a, 8c and 8f (MICs 2.1, 8.0 and 8.1 μM, respectively). In addition, 8a, 8c and 8f demonstrated potent in vitro activity against multidrug-resistant clinical isolates (CDCT-16 and CDCT-27) with promising MIC values ranging from 0.8 to 3.1 μM. Importantly, compounds 8a and 8c were found to be non-toxic against the Vero cell line. The SI value of 8a (>23.8) was found to be comparable to that of isoniazid (>22.7), which suggests the possibility of carrying out advanced studies on this derivative. Therefore, these menadione-derived selenoesters obtained as hybrid compounds represent promising new anti-tubercular agents to overcome TB multidrug resistance., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier Masson SAS. All rights reserved.)

Published

2021

2. Advancing Immunotherapeutic Vaccine Strategies Against Pulmonary Tuberculosis.

Author

Afkhami S, Villela AD, D'Agostino MR, Jeyanathan M, Gillgrass A, and Xing Z

Subjects

Animals, Antitubercular Agents pharmacology, Antitubercular Agents therapeutic use, Drug Resistance, Multiple, Bacterial, Humans, Immunotherapy, Mycobacterium tuberculosis physiology, Precision Medicine, Respiratory Mucosa immunology, Respiratory Mucosa metabolism, Tuberculosis Vaccines administration & dosage, Vaccines, Synthetic administration & dosage, Vaccines, Synthetic immunology, Vaccinology methods, Mycobacterium tuberculosis immunology, Tuberculosis Vaccines immunology, Tuberculosis, Pulmonary prevention & control

Abstract

Chemotherapeutic intervention remains the primary strategy in treating and controlling tuberculosis (TB). However, a complex interplay between therapeutic and patient-related factors leads to poor treatment adherence. This in turn continues to give rise to unacceptably high rates of disease relapse and the growing emergence of drug-resistant forms of TB. As such, there is considerable interest in strategies that simultaneously improve treatment outcome and shorten chemotherapy duration. Therapeutic vaccines represent one such approach which aims to accomplish this through boosting and/or priming novel anti-TB immune responses to accelerate disease resolution, shorten treatment duration, and enhance treatment success rates. Numerous therapeutic vaccine candidates are currently undergoing pre-clinical and clinical assessment, showing varying degrees of efficacy. By dissecting the underlying mechanisms/correlates of their successes and/or shortcomings, strategies can be identified to improve existing and future vaccine candidates. This mini-review will discuss the current understanding of therapeutic TB vaccine candidates, and discuss major strategies that can be implemented in advancing their development., (Copyright © 2020 Afkhami, Villela, D’Agostino, Jeyanathan, Gillgrass and Xing.)

Published

2020

3. Nonclinical evaluation of IQG-607, an anti-tuberculosis candidate with potential use in combination drug therapy.

Author

Rodrigues-Junior VS, Villela AD, Abbadi BL, Sperotto NDM, Pissinate K, Picada JN, Bondan da Silva J, Bizarro CV, Machado P, and Basso LA

Subjects

Animals, Anti-Bacterial Agents administration & dosage, Anti-Bacterial Agents adverse effects, Chromosome Aberrations, Cytochrome P-450 Enzyme System metabolism, Disease Models, Animal, Drug Therapy, Combination, Enzyme Inhibitors administration & dosage, Enzyme Inhibitors adverse effects, Ferrous Compounds administration & dosage, Isoniazid administration & dosage, Isoniazid adverse effects, Isoniazid pharmacology, Male, Mice, Microbial Sensitivity Tests, Mutagenicity Tests, Mycobacterium tuberculosis genetics, Salmonella typhimurium genetics, Tuberculosis microbiology, Anti-Bacterial Agents pharmacology, Enzyme Inhibitors pharmacology, Ferrous Compounds adverse effects, Ferrous Compounds pharmacology, Isoniazid analogs & derivatives, Mycobacterium tuberculosis drug effects, Salmonella typhimurium drug effects, Tuberculosis drug therapy

Abstract

New effective compounds to treat tuberculosis are urgently needed. IQG-607 is an orally active anti-tuberculosis drug candidate, with promising preliminary safety profile and anti-mycobacterial activity in both in vitro and in vivo models of tuberculosis infection. Here, we evaluated the mutagenic and genotoxic effects of IQG-607, and its interactions with CYP450 isoforms. Moreover, we describe for the first time a combination study of IQG-607 in Mycobacterium tuberculosis-infected mice. Importantly, IQG-607 had additive effects when combined with the first-line anti-tuberculosis drugs rifampin and pyrazinamide in mice. IQG-607 presented weak to moderate inhibitory potential against CYP450 isoforms 3A4, 1A2, 2C9, 2C19, 2D6, and 2E1. The Salmonella mutagenicity test revealed that IQG-607 induced base pair substitution mutations in the strains TA100 and TA1535. However, in the presence of human metabolic S9 fraction, no mutagenic effect was detected in any strain. Additionally, IQG-607 did not increase micronucleus frequencies in mice, at any dose tested, 25, 100, or 250 mg/kg. The favorable activity in combination with first-line drugs and mild to moderate toxic events described in this study suggest that IQG-607 represents a candidate for clinical development., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2020

4. Pre-clinical evaluation of quinoxaline-derived chalcones in tuberculosis.

Author

Muradás TC, Abbadi BL, Villela AD, Macchi FS, Bergo PF, de Freitas TF, Sperotto NDM, Timmers LFSM, Norberto de Souza O, Picada JN, Fachini J, da Silva JB, de Albuquerque NCP, Habenschus MD, Carrão DB, Rocha BA, Barbosa Junior F, de Oliveira ARM, Mascarello A, Neuenfeldf P, Nunes RJ, Morbidoni HR, Campos MM, Basso LA, and Rodrigues-Junior VS

Subjects

Bacterial Proteins genetics, Catalase genetics, Cytochrome P-450 CYP2C19 genetics, Cytochrome P-450 CYP2C9 genetics, Cytochrome P-450 CYP3A genetics, Cytochrome P-450 Enzyme System genetics, Humans, Microbial Sensitivity Tests, Mutation, Mycobacterium tuberculosis pathogenicity, Mycolic Acids antagonists & inhibitors, Oxidoreductases genetics, Quinoxalines pharmacology, Tuberculosis genetics, Tuberculosis microbiology, Tuberculosis pathology, Antitubercular Agents pharmacology, Chalcones pharmacology, Mycobacterium tuberculosis drug effects, Tuberculosis drug therapy

Abstract

New effective compounds for tuberculosis treatment are needed. This study evaluated the effects of a series of quinoxaline-derived chalcones against laboratorial strains and clinical isolates of M. tuberculosis. Six molecules, namely N5, N9, N10, N15, N16, and N23 inhibited the growth of the M. tuberculosis H37Rv laboratorial strain. The three compounds (N9, N15 and N23) with the lowest MIC values were further tested against clinical isolates and laboratory strains with mutations in katG or inhA genes. From these data, N9 was selected as the lead compound for further investigation. Importantly, this chalcone displayed a synergistic effect when combined with moxifloxacin. Noteworthy, the anti-tubercular effects of N9 did not rely on inhibition of mycolic acids synthesis, circumventing important mechanisms of resistance. Interactions with cytochrome P450 isoforms and toxic effects were assessed in silico and in vitro. The chalcone N9 was not predicted to elicit any mutagenic, genotoxic, irritant, or reproductive effects, according to in silico analysis. Additionally, N9 did not cause mutagenicity or genotoxicity, as revealed by Salmonella/microsome and alkaline comet assays, respectively. Moreover, N9 did not inhibit the cytochrome P450 isoforms CYP3A4/5, CYP2C9, and CYP2C19. N9 can be considered a potential lead molecule for development of a new anti-tubercular therapeutic agent., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

5. 1H-Benzo[d]imidazoles and 3,4-dihydroquinazolin-4-ones: Design, synthesis and antitubercular activity.

Author

Macchi FS, Pissinate K, Villela AD, Abbadi BL, Rodrigues-Junior V, Nabinger DD, Altenhofen S, Sperotto N, da Silva Dadda A, Subtil FT, de Freitas TF, Erhart Rauber AP, Borsoi AF, Bonan CD, Bizarro CV, Basso LA, Santos DS, and Machado P

Subjects

Animals, Antitubercular Agents chemical synthesis, Antitubercular Agents chemistry, Benzimidazoles chemical synthesis, Benzimidazoles chemistry, Dose-Response Relationship, Drug, Microbial Sensitivity Tests, Molecular Structure, Quinazolinones chemical synthesis, Quinazolinones chemistry, Structure-Activity Relationship, Zebrafish, Antitubercular Agents pharmacology, Benzimidazoles pharmacology, Mycobacterium tuberculosis drug effects, Quinazolinones pharmacology

Abstract

Using a classical hybridization approach, a series of 1H-benzo[d]imidazoles and 3,4-dihydroquinazolin-4-ones were synthesized (39 examples) and evaluated as inhibitors of Mycobacterium tuberculosis growth. Chemical modification studies yielded potent antitubercular agents with minimum inhibitory concentration (MIC) values as low as 0.24 μM against M. tuberculosis H37Rv strain. Further, the synthesized compounds were active against four drug-resistant strains containing different levels of resistance for the first line drugs. These molecules were devoid of apparent toxicity to HepG2, HaCat, and Vero cells with IC 50s  > 30 μM. Viability in mammalian cell cultures was evaluated using MTT and neutral red assays. In addition, some 3,4-dihydroquinazolin-4-ones showed low risk of cardiac toxicity, no signals of neurotoxicity or morphological alteration in zebrafish (Danio rerio) toxicity models. 3,4-Dihydroquinazolin-4-ones 9q and 9w were considered the lead compounds of these series of molecules with MIC values of 0.24 μM and 0.94 μM against M. tuberculosis H37Rv, respectively. Taken together, these data indicate that this class of compounds may furnish candidates for future development of novel anti-TB drugs., (Copyright © 2018 Elsevier Masson SAS. All rights reserved.)

Published

2018

6. Assessing the role of deoD gene in Mycobacterium tuberculosis in vitro growth and macrophage infection.

Author

Dalberto PF, Rodrigues-Junior V, Almeida Falcão VC, Pinto AFM, Abbadi BL, Bizarro CV, Basso LA, Villela AD, and Santos DS

Subjects

Animals, Base Sequence, Chromatography, Liquid, DNA, Bacterial genetics, Gene Expression Profiling, Gene Expression Regulation, Bacterial, Gene Knockdown Techniques, Genes, Bacterial genetics, Mice, Mycobacterium tuberculosis pathogenicity, Oxygen metabolism, RAW 264.7 Cells, Tandem Mass Spectrometry, Tuberculosis microbiology, Macrophages microbiology, Mycobacterium tuberculosis enzymology, Mycobacterium tuberculosis genetics, Mycobacterium tuberculosis growth & development, Purine-Nucleoside Phosphorylase genetics, Purine-Nucleoside Phosphorylase physiology

Abstract

Purine nucleoside phosphorylase from Mycobacterium tuberculosis (MtPNP), encoded by deoD gene (Rv3307), is an enzyme from the purine salvage pathway, which has been widely studied as a molecular target for the development of inhibitors with potential antimycobacterial activity. However, the role of MtPNP in tuberculosis pathogenesis and dormancy is still unknown. The present work aims to construct a deoD knockout strain from M. tuberculosis, to evaluate the role of MtPNP in the growth of M. tuberculosis under oxygenated condition and in a dormancy model, and to assess whether deoD gene is important for M. tuberculosis invasion and growth in macrophages. The construction of a knockout strain for deoD gene was confirmed at DNA level by PCR and protein level by Western blot and LC-MS/MS. The deoD gene is not required for M. tuberculosis growth and survival under oxygenated and hypoxic conditions. The disruption of deoD gene did not affect mycobacterial ability to invade and grow in RAW 264.7 cells under the experimental conditions employed here., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

7. Is IQG-607 a Potential Metallodrug or Metallopro-Drug With a Defined Molecular Target in Mycobacterium tuberculosis ?

Author

Abbadi BL, Rodrigues-Junior VDS, Dadda ADS, Pissinate K, Villela AD, Campos MM, Lopes LGF, Bizarro CV, Machado P, Sousa EHS, and Basso LA

Abstract

The emergence of strains of Mycobacterium tuberculosis resistant to isoniazid (INH) has underscored the need for the development of new anti-tuberculosis agents. INH is activated by the mycobacterial katG -encoded catalase-peroxidase, forming an acylpyridine fragment that is covalently attached to the C4 of NADH. This isonicotinyl-NAD adduct inhibits the activity of 2- trans -enoyl-ACP(CoA) reductase (InhA), which plays a role in mycolic acid biosynthesis. A metal-based INH analog, Na 3 [Fe II (CN) 5 (INH)]·4H 2 O, IQG-607, was designed to have an electronic redistribution on INH moiety that would lead to an intramolecular electron transfer to bypass KatG activation. HPLC and EPR studies showed that the INH moiety can be oxidized by superoxide or peroxide yielding similar metabolites and isonicotinoyl radical only when associated to IQG-607, thereby supporting redox-mediated drug activation as a possible mechanism of action. However, IQG-607 was shown to inhibit the in vitro activity of both wild-type and INH-resistant mutant InhA enzymes in the absence of KatG activation. IQG-607 given by the oral route to M. tuberculosis -infected mice reduced lung lesions. Experiments using early and late controls of infection revealed a bactericidal activity for IQG-607. HPLC and voltammetric methods were developed to quantify IQG-607. Pharmacokinetic studies showed short half-life, high clearance, moderate volume of distribution, and low oral bioavailability, which was not altered by feeding. Safety and toxic effects of IQG-607 after acute and 90-day repeated oral administrations in both rats and minipigs showed occurrence of mild to moderate toxic events. Eight multidrug-resistant strains (MDR-TB) were resistant to IQG-607, suggesting an association between katG mutation and increasing MIC values. Whole genome sequencing of three spontaneous IQG-607-resistant strains harbored katG gene mutations. MIC measurements and macrophage infection experiments with a laboratorial strain showed that katG mutation is sufficient to confer resistance to IQG-607 and that the macrophage intracellular environment cannot trigger the self-activation mechanism. Reduced activity of IQG-607 against an M. tuberculosis strain overexpressing S94A InhA mutant protein suggested both the need for KatG activation and InhA as its target. Further efforts are suggested to be pursued toward attempting to translate IQG-607 into a chemotherapeutic agent to treat tuberculosis.

Published

2018

8. Activity of 2-(quinolin-4-yloxy)acetamides in Mycobacterium tuberculosis clinical isolates and identification of their molecular target by whole-genome sequencing.

Author

Subtil FT, Villela AD, Abbadi BL, Rodrigues-Junior VS, Bizarro CV, Timmers LFSM, de Souza ON, Pissinate K, Machado P, López-Gavín A, Tudó G, González-Martín J, Basso LA, and Santos DS

Subjects

DNA Mutational Analysis, Humans, Microbial Sensitivity Tests, Mycobacterium tuberculosis isolation & purification, Tuberculosis microbiology, Whole Genome Sequencing, Antitubercular Agents pharmacology, Electron Transport Complex III antagonists & inhibitors, Mycobacterium tuberculosis drug effects, Quinolines pharmacology

Abstract

The 2-(quinolin-4-yloxy)acetamides (QOAs) have been reported to be promising molecules for tuberculosis treatment. Recent studies demonstrated their potent antimycobacterial activity, biological stability and synergism with rifampicin. The identification of the molecular target is an essential step towards the development of a novel drug candidate. Here, we report the target identification of the QOAs. We found that these compounds are active against Mycobacterium tuberculosis clinical isolates resistant to isoniazid, rifampicin, ethambutol, streptomycin and ethionamide. The initial evidence that DNA gyrase might be the target of QOAs, based on high minimum inhibitory concentration (MIC) values against ofloxacin-resistant clinical isolates and structural similarities with fluoroquinolones, was discarded by experiments performed with M. tuberculosis GyrA point mutant, DNA gyrase supercoiling inhibition assay and overexpression of DNA gyrase. We selected spontaneous mutants for our lead compound 21 and observed that these strains were also resistant to all QOA derivatives. The genomes of the spontaneous mutants were sequenced, and the results revealed a single mutation in qcrB gene (T313A), which indicates that the QOAs target the cytochrome bc 1 complex. The protein-compound interaction was further investigated by molecular docking. These findings reinforce the relevance of these compounds as promising candidates for the treatment of multidrug-resistant tuberculosis., (Copyright © 2017 Elsevier B.V. and International Society of Chemotherapy. All rights reserved.)

Published

2018

9. Effect of the bradykinin 1 receptor antagonist SSR240612 after oral administration in Mycobacterium tuberculosis-infected mice.

Author

Rodrigues-Junior VS, Pail PB, Villela AD, Falcão VCA, Dadda AS, Abbadi BL, Pesquero JB, Santos DS, Basso LA, and Campos MM

Subjects

Administration, Oral, Animals, Bacterial Load, Bradykinin administration & dosage, Bradykinin analogs & derivatives, Bradykinin B2 Receptor Antagonists administration & dosage, Disease Models, Animal, Female, Lung metabolism, Lung microbiology, Macrophages drug effects, Macrophages metabolism, Macrophages microbiology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Mycobacterium tuberculosis growth & development, RAW 264.7 Cells, Receptor, Bradykinin B1 deficiency, Receptor, Bradykinin B1 genetics, Receptor, Bradykinin B1 metabolism, Receptor, Bradykinin B2 genetics, Receptor, Bradykinin B2 metabolism, Spleen drug effects, Spleen metabolism, Spleen microbiology, Tuberculosis, Pulmonary genetics, Tuberculosis, Pulmonary metabolism, Tuberculosis, Pulmonary microbiology, Antitubercular Agents administration & dosage, Bradykinin B1 Receptor Antagonists administration & dosage, Dioxoles administration & dosage, Lung drug effects, Mycobacterium tuberculosis drug effects, Receptor, Bradykinin B1 drug effects, Sulfonamides administration & dosage, Tuberculosis, Pulmonary drug therapy

Abstract

The role, if any, played by the kinin system in tuberculosis infection models, either in vivo or in vitro, was investigated. The effects of Mycobacterium tuberculosis infection on C57BL/6 wild type, B 1 R-/-, B 2 R-/- and double B 1 R/B 2 R knockout mice were evaluated. Immunohistochemistry analysis was carried out to assess B 1 R and B 2 R expression in spleens and lungs of M. tuberculosis-infected mice. In addition, in vitro experiments with M. tuberculosis-infected macrophages were performed. The in vivo effects of HOE-140 and SSR240612 on the mice model of infection were also evaluated. Infected B 2 R-/- mice exhibited increased splenomegaly, whereas decreased spleen weight in infected double B 1 R/B 2 R knockout mice was observed. The bacterial load, determined as colony-forming units, did not differ in the spleens and lungs of the studied mouse strains. Importantly, immunohistochemical analysis revealed that B 1 R was upregulated in both spleens and lungs of infected mice. M. tuberculosis-infected macrophages incubated with SSR240612, alone or in combination with des-Arg 9 -BK, for four days, displayed a marked inhibitory effect on CFU counts. However, the pre-incubation of the selective B 1 R (des-Arg 9 -BK and SSR240612) and B 2 R (BK and HOE-140) agonists and antagonists, respectively, did not significantly affect the bacterial loads. A statistically significant reduction in the CFU of M. tuberculosis in lungs and spleens of animals treated with SSR240612, but not with HOE-140, was observed. Further efforts should be pursued to clarify whether or not SSR240612 might be considered an option for the treatment of tuberculosis., (Copyright © 2018. Published by Elsevier Ltd.)

Published

2018

10. Synthesis and mechanistic investigation of iron(II) complexes of isoniazid and derivatives as a redox-mediated activation strategy for anti-tuberculosis therapy.

Author

Laborde J, Deraeve C, de Mesquita Vieira FG, Sournia-Saquet A, Rechignat L, Villela AD, Abbadi BL, Macchi FS, Pissinate K, Bizarro CV, Machado P, Basso LA, Pratviel G, de França Lopes LG, Sousa EHS, and Bernardes-Génisson V

Subjects

Antitubercular Agents chemical synthesis, Antitubercular Agents chemistry, Coordination Complexes chemical synthesis, Coordination Complexes chemistry, Ferrous Compounds chemical synthesis, Ferrous Compounds chemistry, Isoniazid chemical synthesis, Isoniazid chemistry, Microbial Sensitivity Tests, Models, Chemical, Mycobacterium tuberculosis drug effects, Oxidation-Reduction, Antitubercular Agents pharmacology, Coordination Complexes pharmacology, Ferrous Compounds pharmacology, Isoniazid analogs & derivatives, Isoniazid pharmacology

Abstract

The emergence of multidrug-resistant strains of Mycobacterium tuberculosis (MTB) represents a major threat to global health. Isoniazid (INH) is a prodrug used in the first-line treatment of tuberculosis. It undergoes oxidation by a catalase-peroxidase KatG, leading to generation of an isonicotinoyl radical that reacts with NAD(H) forming the INH-NADH adduct as the active metabolite. A redox-mediated activation of isoniazid using an iron metal complex was previously proposed as a strategy to overcome isoniazid resistance due to KatG mutations. Here, we have prepared a series of iron metal complexes with isoniazid and analogues, containing alkyl substituents at the hydrazide moiety, and also with pyrazinamide derivatives. These complexes were activated by H 2 O 2 and studied by ESR and LC-MS. For the first time, the formation of the oxidized INH-NAD adduct from the pentacyano(isoniazid)ferrate(II) complex was detected by LC-MS, supporting a redox-mediated activation, for which a mechanistic proposition is reported. ESR data showed all alkylated hydrazides, in contrast to non-substituted hydrazides, only generated alkyl-based radicals. The structural modifications did not improve minimal inhibitory concentration (MIC) against MTB in comparison to isoniazid iron complex, providing support to isonicotinoyl radical formation as a requirement for activity. Nonetheless, the pyrazinoic acid hydrazide iron complex showed redox-mediated activation using H 2 O 2 with generation of a pyrazinoyl radical intermediate and production of pyrazinoic acid, which is in fact the active metabolite of pyrazinamide prodrug. Thereby, this strategy can also unveil new opportunities for activation of this type of drug., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2018

11. Revisiting Activation of and Mechanism of Resistance to Compound IQG-607 in Mycobacterium tuberculosis.

Author

Abbadi BL, Villela AD, Rodrigues-Junior VS, Subtil FT, Dalberto PF, Pinheiro APS, Santos DS, Machado P, Basso LA, and Bizarro CV

Subjects

Bacterial Proteins genetics, DNA, Bacterial genetics, Drug Resistance, Bacterial genetics, Humans, Isoniazid pharmacology, Mutation genetics, Mycobacterium tuberculosis genetics, Whole Genome Sequencing methods, Antitubercular Agents pharmacology, Drug Resistance, Bacterial drug effects, Ferrous Compounds pharmacology, Isoniazid analogs & derivatives, Mycobacterium tuberculosis drug effects, Tuberculosis, Multidrug-Resistant drug therapy

Abstract

IQG-607 is a metal complex previously reported as a promising anti-tuberculosis (TB) drug against isoniazid (INH)-resistant strains of Mycobacterium tuberculosis Unexpectedly, we found that INH-resistant clinical isolates were resistant to IQG-607. Spontaneous mutants resistant to IQG-607 were subjected to whole-genome sequencing, and all sequenced colonies carried alterations in the katG gene. The katG (S315T) mutation was sufficient to confer resistance to IQG-607 in both MIC assays and inside macrophages. Moreover, overexpression of the InhA(S94A) protein caused IQG-607's resistance., (Copyright © 2018 American Society for Microbiology.)

Published

2018

12. Construction of Mycobacterium tuberculosis cdd knockout and evaluation of invasion and growth in macrophages.

Author

Villela AD, Rodrigues-Junior VS, Pinto AFM, Falcão VCA, Sánchez-Quitian ZA, Eichler P, Bizarro CV, Basso LA, and Santos DS

Subjects

Cytidine Deaminase biosynthesis, Deoxycytidine biosynthesis, Gene Knockout Techniques, Humans, Mycobacterium tuberculosis enzymology, Mycobacterium tuberculosis growth & development, Time Factors, Cytidine Deaminase genetics, Deoxycytidine genetics, Macrophages microbiology, Mycobacterium tuberculosis pathogenicity

Abstract

Cytidine deaminase (MtCDA), encoded by cdd gene (Rv3315c), is the only enzyme identified in nucleotide biosynthesis pathway of Mycobacterium tuberculosis that is able to recycle cytidine and deoxycytidine. An M. tuberculosis knockout strain for cdd gene was obtained by allelic replacement. Evaluation of mRNA expression validated cdd deletion and showed the absence of polar effect. MudPIT LC-MS/MS data indicated thymidine phosphorylase expression was decreased in knockout and complemented strains. The cdd disruption does not affect M. tuberculosis growth both in Mid- dlebrook 7H9 and in RAW 264.7 cells, which indicates that cdd is not important for macrophage invasion and virulence.

Published

2017

13. Functional, thermodynamics, structural and biological studies of in silico-identified inhibitors of Mycobacterium tuberculosis enoyl-ACP(CoA) reductase enzyme.

Author

Martinelli LKB, Rotta M, Villela AD, Rodrigues-Junior VS, Abbadi BL, Trindade RV, Petersen GO, Danesi GM, Nery LR, Pauli I, Campos MM, Bonan CD, de Souza ON, Basso LA, and Santos DS

Subjects

Animals, Antitubercular Agents pharmacology, Bacterial Proteins metabolism, Cell Line, Chlorocebus aethiops, Humans, Kinetics, Mice, Microbial Sensitivity Tests, Mycobacterium tuberculosis enzymology, Mycobacterium tuberculosis physiology, Oxidoreductases metabolism, RAW 264.7 Cells, Tuberculosis microbiology, Vero Cells, Bacterial Proteins antagonists & inhibitors, Computer Simulation, Enzyme Inhibitors pharmacology, Mycobacterium tuberculosis drug effects, Oxidoreductases antagonists & inhibitors, Thermodynamics

Abstract

Novel chemotherapeutics agents are needed to kill Mycobacterium tuberculosis, the main causative agent of tuberculosis (TB). The M. tuberculosis 2-trans-enoyl-ACP(CoA) reductase enzyme (MtInhA) is the druggable bona fide target of isoniazid. New chemotypes were previously identified by two in silico approaches as potential ligands to MtInhA. The inhibition mode was determined by steady-state kinetics for seven compounds that inhibited MtInhA activity. Dissociation constant values at different temperatures were determined by protein fluorescence spectroscopy. van't Hoff analyses of ligand binding to MtInhA:NADH provided the thermodynamic signatures of non-covalent interactions (ΔH°, ΔS°, ΔG°). Phenotypic screening showed that five compounds inhibited in vitro growth of M. tuberculosis H37Rv strain. Labio_16 and Labio_17 compounds also inhibited the in vitro growth of PE-003 multidrug-resistant strain. Cytotoxic effects on Hacat, Vero and RAW 264.7 cell lines were assessed for the latter two compounds. The Labio_16 was bacteriostatic and Labio_17 bactericidal in an M. tuberculosis-infected macrophage model. In Zebrafish model, Labio_16 showed no cardiotoxicity whereas Labio_17 showed dose-dependent cardiotoxicity. Accordingly, a model was built for the MtInhA:NADH:Labio_16 ternary complex. The results show that the Labio_16 compound is a direct inhibitor of MtInhA, and it may represent a hit for the development of chemotherapeutic agents to treat TB.

Published

2017

14. Validation of Mycobacterium tuberculosis dihydroneopterin aldolase as a molecular target for anti-tuberculosis drug development.

Author

Falcão VC, Villela AD, Rodrigues-Junior VS, Pissinate K, Eichler P, Pinto AF, Basso LA, Santos DS, and Bizarro CV

Subjects

Aldehyde-Lyases genetics, Aldehyde-Lyases metabolism, Bacterial Proteins genetics, Bacterial Proteins metabolism, Biocatalysis, Chromatography, High Pressure Liquid, Genes, Essential genetics, Genetic Complementation Test methods, Humans, Microbial Viability drug effects, Microbial Viability genetics, Molecular Targeted Therapy methods, Mutation, Missense, Mycobacterium tuberculosis enzymology, Mycobacterium tuberculosis genetics, Reproducibility of Results, Substrate Specificity, Tandem Mass Spectrometry, Tuberculosis drug therapy, Tuberculosis microbiology, Aldehyde-Lyases antagonists & inhibitors, Antitubercular Agents pharmacology, Bacterial Proteins antagonists & inhibitors, Drug Discovery methods, Mycobacterium tuberculosis drug effects

Abstract

An early step of target validation in antimicrobial drug discovery is to prove that a gene coding for a putative target is essential for pathogen's viability. However, little attention has been paid to demonstrate the causal links between gene essentiality and a particular protein function that will be the focus of a drug discovery effort. This should be considered an important step in target validation since a growing number of proteins are found to exhibit multiple and unrelated tasks. Here, we show that the Mycobacterium tuberculosis (Mtb) folB gene is essential and that this essentiality depends on the dihydroneopterin aldolase/epimerase activities of its protein product, the FolB protein from the folate biosynthesis pathway. The wild-type (WT) MtFolB and point mutants K99A and Y54F were cloned, expressed, purified and monitored for the aldolase, epimerase and oxygenase activities using HPLC. In contrast to the WT MtFolB, both mutants have neither aldolase nor epimerase activities in the conditions assayed. We then performed gene knockout experiments and showed that folB gene is essential for Mtb survival under the conditions tested. Moreover, only the WT folB sequence could be used as a rescue copy in gene complementation studies. When the sequences of mutants K99A or Y54F were used for complementation, no viable colonies were obtained, indicating that aldolase and/or epimerase activities are crucial for Mtb survival. These results provide a solid basis for further work aiming to develop new anti-TB agents acting as inhibitors of the aldolase/epimerase activities of MtFolB., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

15. Characterisation of iunH gene knockout strain from Mycobacterium tuberculosis.

Author

Villela AD, Rodrigues VD Junior, Pinto AF, Wink PL, Sánchez-Quitian ZA, Petersen GO, Campos MM, Basso LA, and Santos DS

Subjects

Humans, Macrophages microbiology, Mycobacterium tuberculosis enzymology, Mycobacterium tuberculosis growth & development, Gene Knockout Techniques, Genes, Bacterial, Mycobacterium tuberculosis genetics, N-Glycosyl Hydrolases genetics

Abstract

Background: Tuberculosis (TB) is an infectious disease caused mainly by the bacillus Mycobacterium tuberculosis. The better understanding of important metabolic pathways from M. tuberculosis can contribute to the development of novel therapeutic and prophylactic strategies to combat TB. Nucleoside hydrolase (MtIAGU-NH), encoded by iunH gene (Rv3393), is an enzyme from purine salvage pathway in M. tuberculosis. MtIAGU-NH accepts inosine, adenosine, guanosine, and uridine as substrates, which may point to a pivotal metabolic role., Objectives: Our aim was to construct a M. tuberculosis knockout strain for iunH gene, to evaluate in vitro growth and the effect of iunH deletion in M. tuberculosis in non-activated and activated macrophages models of infection., Methods: A M. tuberculosis knockout strain for iunH gene was obtained by allelic replacement, using pPR27xylE plasmid. The complemented strain was constructed by the transformation of the knockout strain with pNIP40::iunH. MtIAGU-NH expression was analysed by Western blot and LC-MS/MS. In vitro growth was evaluated in Sauton's medium. Bacterial load of non-activated and interferon-γ activated RAW 264.7 cells infected with knockout strain was compared with wild-type and complemented strains., Findings: Western blot and LC-MS/MS validated iunH deletion at protein level. The iunH knockout led to a delay in M. tuberculosis growth kinetics in Sauton's medium during log phase, but did not affect bases and nucleosides pool in vitro. No significant difference in bacterial load of knockout strain was observed when compared with both wild-type and complemented strains after infection of non-activated and interferon-γ activated RAW 264.7 cells., Main Conclusion: The disruption of iunH gene does not influence M. tuberculosis growth in both non-activated and activated RAW 264.7 cells, which show that iunH gene is not important for macrophage invasion and virulence. Our results indicated that MtIAGU-NH is not a target for drug development.

Published

2017

16. Analysis of uracil phosphoribosyltransferase expression in Mycobacterium tuberculosis and evaluation of upp knockout strain in infected mice.

Author

Villela AD, Pham H, Jones V, Grzegorzewicz AE, Rodrigues-Junior VD, Campos MM, Basso LA, Jackson M, and Santos DS

Subjects

Animals, Bacterial Proteins genetics, Bacterial Proteins metabolism, Disease Models, Animal, Gene Knockout Techniques, Mice, Mycobacterium tuberculosis genetics, Mycobacterium tuberculosis growth & development, Pentosyltransferases metabolism, Uracil metabolism, Uracil pharmacology, Virulence, Gene Expression, Mycobacterium tuberculosis enzymology, Mycobacterium tuberculosis pathogenicity, Pentosyltransferases genetics, Tuberculosis microbiology

Abstract

The upp (Rv3309c)-encoded uracil phosphoribosyltransferase from Mycobacterium tuberculosis (MtUPRT) converts uracil and 5-phosphoribosyl-α-1-pyrophosphate into pyrophosphate and uridine 5΄-monophosphate, the precursor of all pyrimidine nucleotides. A M. tuberculosis knockout strain for upp gene was generated by allelic replacement. Knockout and complemented strains were validated by a functional assay of uracil incorporation. A basal level of MtUPRT expression is shown to be independent of either growth medium used, addition of bases, or oxygen presence/absence. The upp disruption does not affect M. tuberculosis growth in Middlebrook 7H9 medium, and it is not required for M. tuberculosis virulence in a mouse model of infection. Thus, MtUPRT is unlikely to be a good target for drugs against M. tuberculosis., (© FEMS 2017. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2017

17. New insights into the SAR and drug combination synergy of 2-(quinolin-4-yloxy)acetamides against Mycobacterium tuberculosis.

Author

Giacobbo BC, Pissinate K, Rodrigues-Junior V, Villela AD, Grams ES, Abbadi BL, Subtil FT, Sperotto N, Trindade RV, Back DF, Campos MM, Basso LA, Machado P, and Santos DS

Subjects

Acetamides chemical synthesis, Acetamides metabolism, Animals, Antitubercular Agents chemical synthesis, Antitubercular Agents metabolism, Drug Resistance, Bacterial drug effects, Drug Synergism, Humans, Macrophages drug effects, Macrophages microbiology, Mice, Microbial Sensitivity Tests, RAW 264.7 Cells, Structure-Activity Relationship, Acetamides chemistry, Acetamides pharmacology, Antitubercular Agents chemistry, Antitubercular Agents pharmacology, Mycobacterium tuberculosis drug effects, Quinolines chemistry

Abstract

2-(Quinolin-4-yloxy)acetamides have been described as potent and selective in vitro inhibitors of Mycobacterium tuberculosis (Mtb) growth. Herein, a new series of optimized compounds were found to demonstrate highly potent antitubercular activity, with minimum inhibitory concentration (MIC) values against drug-susceptible and drug-resistant Mycobacterium tuberculosis strains in the submicromolar range. Furthermore, the most active compounds had no apparent toxicity to mammalian cells, and they showed intracellular activities similar to those of isoniazid and rifampin in a macrophage model of Mtb infection. Use of the checkerboard method to investigate the association profiles of lead compounds with first- and second-line antituberculosis drugs showed that 2-(quinolin-4-yloxy)acetamides have a synergistic effect with rifampin. Ultimately, the good permeability, moderate rates of metabolism and low risk of drug-drug interactions displayed by some of the synthesized compounds indicate that 2-(quinolin-4-yloxy)acetamides may yield candidates to use in the development of novel alternative therapeutics for tuberculosis treatment., (Copyright © 2016 Elsevier Masson SAS. All rights reserved.)

Published

2017

18. Mefloquine and its oxazolidine derivative compound are active against drug-resistant Mycobacterium tuberculosis strains and in a murine model of tuberculosis infection.

Author

Rodrigues-Junior VS, Villela AD, Gonçalves RS, Abbadi BL, Trindade RV, López-Gavín A, Tudó G, González-Martín J, Basso LA, de Souza MV, Campos MM, and Santos DS

Subjects

Animals, Bacterial Load, Disease Models, Animal, Drug Interactions, Drug Repositioning, Male, Mice, Microbial Sensitivity Tests, Tuberculosis, Multidrug-Resistant drug therapy, Tuberculosis, Multidrug-Resistant microbiology, Antitubercular Agents pharmacology, Antitubercular Agents therapeutic use, Mefloquine pharmacology, Mefloquine therapeutic use, Mycobacterium tuberculosis drug effects, Oxazoles pharmacology, Oxazoles therapeutic use

Abstract

Repurposing of drugs to treat tuberculosis (TB) has been considered an alternative to overcome the global TB epidemic, especially to combat drug-resistant forms of the disease. Mefloquine has been reported as a potent drug to kill drug-resistant strains of Mycobacterium tuberculosis. In addition, mefloquine-derived molecules have been synthesised and their effectiveness against mycobacteria has been assessed. In this work, we demonstrate for the first time the activities of mefloquine and its oxazolidine derivative compound 1E in a murine model of TB infection following administration of both drugs by the oral route. The effects of associations between mefloquine or 1E with the clinically used antituberculosis drugs isoniazid, rifampicin, ethambutol, moxifloxacin and streptomycin were also investigated. Importantly, combination of mefloquine with isoniazid and of 1E with streptomycin showed a two-fold decrease in their minimum inhibitory concentrations (MICs). Moreover, no tested combinations demonstrated antagonist interactions. Here we describe novel evidence on the activity of mefloquine and 1E against a series of quinolone-resistant M. tuberculosis strains. These data show MICs against quinolone-resistant strains (0.5-8 µg/mL) similar to or lower than those previously reported for multidrug-resistant strains. Taking these results together, we can suggest the use of mefloquine or 1E in combination with clinically available drugs, especially in the case of resistant forms of TB., (Copyright © 2016 Elsevier B.V. and International Society of Chemotherapy. All rights reserved.)

Published

2016

19. 2-(Quinolin-4-yloxy)acetamides Are Active against Drug-Susceptible and Drug-Resistant Mycobacterium tuberculosis Strains.

Author

Pissinate K, Villela AD, Rodrigues-Junior V, Giacobbo BC, Grams ES, Abbadi BL, Trindade RV, Roesler Nery L, Bonan CD, Back DF, Campos MM, Basso LA, Santos DS, and Machado P

Abstract

2-(Quinolin-4-yloxy)acetamides have been described as potent in vitro inhibitors of Mycobacterium tuberculosis growth. Herein, additional chemical modifications of lead compounds were carried out, yielding highly potent antitubercular agents with minimum inhibitory concentration (MIC) values as low as 0.05 μM. Further, the synthesized compounds were active against drug-resistant strains and were devoid of apparent toxicity to Vero and HaCat cells (IC50s ≥ 20 μM). In addition, the 2-(quinolin-4-yloxy)acetamides showed intracellular activity against the bacilli in infected macrophages with action similar to rifampin, low risk of drug-drug interactions, and no sign of cardiac toxicity in zebrafish (Danio rerio) at 1 and 5 μM. Therefore, these data indicate that this class of compounds may furnish candidates for future development to, hopefully, provide drug alternatives for tuberculosis treatment.

Published

2016

20. Gene replacement and quantitative mass spectrometry approaches validate guanosine monophosphate synthetase as essential for Mycobacterium tuberculosis growth.

Author

Villela AD, Eichler P, Pinto AFM, Rodrigues-Junior V, Yates Iii JR, Bizarro CV, Basso LA, and Santos DS

Abstract

Guanosine monophosphate synthetase (GMPS), encoded by guaA gene, is a key enzyme for guanine nucleotide biosynthesis in Mycobacterium tuberculosis . The guaA gene from several bacterial pathogens has been shown to be involved in virulence; however, no information about the physiological effect of direct guaA deletion in M. tuberculosis has been described so far. Here, we demonstrated that the guaA gene is essential for M. tuberculosis H37Rv growth. The lethal phenotype of guaA gene disruption was avoided by insertion of a copy of the ortholog gene from Mycobacterium smegmatis, indicating that this GMPS protein is functional in M. tuberculosis . Protein validation of the guaA essentiality observed by PCR was approached by shotgun proteomic analysis. A quantitative method was performed to evaluate protein expression levels, and to check the origin of common and unique peptides from M. tuberculosis and M. smegmatis GMPS proteins. These results validate GMPS as a molecular target for drug design against M. tuberculosis , and GMPS inhibitors might prove to be useful for future development of new drugs to treat human tuberculosis.

Published

2015

21. Piperazine derivatives: synthesis, inhibition of the Mycobacterium tuberculosis enoyl-acyl carrier protein reductase and SAR studies.

Author

Rotta M, Pissinate K, Villela AD, Back DF, Timmers LF, Bachega JF, de Souza ON, Santos DS, Basso LA, and Machado P

Subjects

Dose-Response Relationship, Drug, Enoyl-(Acyl-Carrier-Protein) Reductase (NADH) metabolism, Enzyme Activation drug effects, Kinetics, Models, Molecular, Molecular Structure, Piperazine, Piperazines chemical synthesis, Piperazines chemistry, Structure-Activity Relationship, Enoyl-(Acyl-Carrier-Protein) Reductase (NADH) antagonists & inhibitors, Mycobacterium tuberculosis enzymology, Piperazines pharmacology

Abstract

The Mycobacterium tuberculosis NADH-dependent enoyl-acyl carrier protein reductase (MtInhA) catalyzes hydride transfer to long-chain enoyl thioester substrates. MtInhA is a member of the mycobacterial type II dissociated fatty acid biosynthesis system, and is the bona fide target for isoniazid, the most prescribed drug for tuberculosis treatment. Here, a series of piperazine derivatives was synthesized and screened as MtInhA inhibitors, which resulted in the identification of compounds with IC50 values in the submicromolar range. A structure-activity relationship (SAR) evaluation indicated the importance of the chemical environment surrounding the carbonyl group for inhibition. In addition, the structure of one selected compound was supported by crystallographic studies, and experimental geometrical values were compared with semi-empirical quantum chemical calculations. Furthermore, the mode of inhibition and inhibitory dissociation constants were determined for the nine most active compounds. These findings suggest that these 9H-fluoren-9-yl-piperazine-containing compounds interact with MtInhA at the enoyl thioester (2-trans-dodecenoyl-CoA) substrate binding site., (Copyright © 2014 Elsevier Masson SAS. All rights reserved.)

Published

2015

22. Real time PCR quantification of viable Mycobacterium tuberculosis from sputum samples treated with propidium monoazide.

Author

de Assunção TM, Batista EL Jr, Deves C, Villela AD, Pagnussatti VE, de Oliveira Dias AC, Kritski A, Rodrigues-Junior V, Basso LA, and Santos DS

Subjects

Affinity Labels, Azides administration & dosage, Colony Count, Microbial, Coloring Agents administration & dosage, Coloring Agents pharmacology, DNA, Bacterial analysis, DNA, Intergenic genetics, Dose-Response Relationship, Drug, Humans, Microbial Viability, Mycobacterium tuberculosis drug effects, Mycobacterium tuberculosis genetics, Propidium administration & dosage, Propidium pharmacology, Real-Time Polymerase Chain Reaction methods, Sensitivity and Specificity, Azides pharmacology, Mycobacterium tuberculosis isolation & purification, Propidium analogs & derivatives, Sputum microbiology, Tuberculosis, Pulmonary diagnosis

Abstract

Diagnostic methods of TB, nowadays, are prone to delay in diagnosis, increased false negative results and are not sensitive to many forms of paucibacillary disease. The aims of this study were to implement a quantitative nucleic acid-based diagnostic test for paucibacillary tuberculosis, enabling the identification and quantification of viable Mycobacterium tuberculosis bacilli by quantitative Real-Time PCR (qRT-PCR). The intergenic region of the single-copy inhA-mabA gene was chosen as the target region for design of primers and probes conjugated with fluorophores. The construction of synthetic DNA flanking the target region served as standards for absolute quantification of nucleic acids. Using the intercaling dye, propidium monoazide, we were able to discriminate between viable and dead cells of M. tuberculosis. The diagnosis method showed a broad sensitivity (96.1%) when only compared to samples of smear-positive sputum and ROC analyses shows that our approach performed well and yielded a specificity of 84.6% and a sensitivity of 84.6% when compared to M. tuberculosis colony-forming units counting., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

23. IQG-607 abrogates the synthesis of mycolic acids and displays intracellular activity against Mycobacterium tuberculosis in infected macrophages.

Author

Rodrigues-Junior VS, dos Santos Junior AA, Villela AD, Belardinelli JM, Morbidoni HR, Basso LA, Campos MM, and Santos DS

Subjects

Colony Count, Microbial, Humans, Isoniazid pharmacology, Microbial Viability drug effects, Antitubercular Agents pharmacology, Ferrous Compounds pharmacology, Isoniazid analogs & derivatives, Macrophages microbiology, Mycobacterium tuberculosis drug effects, Mycobacterium tuberculosis metabolism, Mycolic Acids antagonists & inhibitors, Mycolic Acids metabolism

Abstract

In this work, the antitubercular activity of a pentacyano(isoniazid)ferrate(II) compound (IQG-607) was investigated using a macrophage model of Mycobacterium tuberculosis infection. Importantly, treatment of M.-tuberculosis-infected macrophages with IQG-607 significantly diminished the number of CFU compared with the untreated control group. The antitubercular activity of IQG-607 was similar to that observed for the positive control drugs isoniazid and rifampicin. Nevertheless, higher concentrations of IQG-607 produced a significantly greater reduction in bacterial load compared with the same concentrations of isoniazid. Analysis of the mechanism of action of IQG-607 revealed that the biosynthesis of mycolic acids was blocked. The promising activity of IQG-607 in infected macrophages and the experimental determination of its mechanism of action may help in further studies aimed at the development of a new antimycobacterial agent., (Copyright © 2013 Elsevier B.V. and the International Society of Chemotherapy. All rights reserved.)

Published

2014

24. Biochemical characterization of uracil phosphoribosyltransferase from Mycobacterium tuberculosis.

Author

Villela AD, Ducati RG, Rosado LA, Bloch CJ, Prates MV, Gonçalves DC, Ramos CH, Basso LA, and Santos DS

Subjects

Allosteric Regulation, Amino Acid Sequence, Hydrogen-Ion Concentration, Kinetics, Molecular Sequence Data, Nucleotides metabolism, Pentosyltransferases genetics, Pentosyltransferases isolation & purification, Polymerase Chain Reaction, Sequence Analysis, Substrate Specificity, Mycobacterium tuberculosis enzymology, Pentosyltransferases chemistry, Pentosyltransferases metabolism

Abstract

Uracil phosphoribosyltransferase (UPRT) catalyzes the conversion of uracil and 5-phosphoribosyl-α-1-pyrophosphate (PRPP) to uridine 5'-monophosphate (UMP) and pyrophosphate (PP(i)). UPRT plays an important role in the pyrimidine salvage pathway since UMP is a common precursor of all pyrimidine nucleotides. Here we describe cloning, expression and purification to homogeneity of upp-encoded UPRT from Mycobacterium tuberculosis (MtUPRT). Mass spectrometry and N-terminal amino acid sequencing unambiguously identified the homogeneous protein as MtUPRT. Analytical ultracentrifugation showed that native MtUPRT follows a monomer-tetramer association model. MtUPRT is specific for uracil. GTP is not a modulator of MtUPRT ativity. MtUPRT was not significantly activated or inhibited by ATP, UTP, and CTP. Initial velocity and isothermal titration calorimetry studies suggest that catalysis follows a sequential ordered mechanism, in which PRPP binding is followed by uracil, and PP(i) product is released first followed by UMP. The pH-rate profiles indicated that groups with pK values of 5.7 and 8.1 are important for catalysis, and a group with a pK value of 9.5 is involved in PRPP binding. The results here described provide a solid foundation on which to base upp gene knockout aiming at the development of strategies to prevent tuberculosis.

Published

2013

25. A small multidrug resistance-like transporter involved in the arabinosylation of arabinogalactan and lipoarabinomannan in mycobacteria.

Author

Larrouy-Maumus G, Škovierová H, Dhouib R, Angala SK, Zuberogoitia S, Pham H, Villela AD, Mikušová K, Noguera A, Gilleron M, Valentínová L, Korduláková J, Brennan PJ, Puzo G, Nigou J, and Jackson M

Subjects

Arabinose genetics, Arabinose metabolism, Bacterial Proteins genetics, Galactans genetics, Genetic Complementation Test, Glycosylation, Lipopolysaccharides genetics, Membrane Transport Proteins genetics, Mutation, Mycobacterium smegmatis genetics, Mycobacterium smegmatis metabolism, Mycobacterium tuberculosis genetics, Bacterial Proteins metabolism, Drug Resistance, Multiple, Bacterial physiology, Galactans metabolism, Lipopolysaccharides metabolism, Membrane Transport Proteins metabolism, Mycobacterium tuberculosis metabolism

Abstract

The biosynthesis of the major cell envelope glycoconjugates of Mycobacterium tuberculosis is topologically split across the plasma membrane, yet nothing is known of the transporters required for the translocation of lipid-linked sugar donors and oligosaccharide intermediates from the cytoplasmic to the periplasmic side of the membrane in mycobacteria. One of the mechanisms used by prokaryotes to translocate lipid-linked phosphate sugars across the plasma membrane relies on translocases that share resemblance with small multidrug resistance transporters. The presence of an small multidrug resistance-like gene, Rv3789, located immediately upstream from dprE1/dprE2 responsible for the formation of decaprenyl-monophosphoryl-β-D-arabinose (DPA) in the genome of M. tuberculosis led us to investigate its potential involvement in the formation of the major arabinosylated glycopolymers, lipoarabinomannan (LAM) and arabinogalactan (AG). Disruption of the ortholog of Rv3789 in Mycobacterium smegmatis resulted in a reduction of the arabinose content of both AG and LAM that accompanied the accumulation of DPA in the mutant cells. Interestingly, AG and LAM synthesis was restored in the mutant not only upon expression of Rv3789 but also upon that of the undecaprenyl phosphate aminoarabinose flippase arnE/F genes from Escherichia coli. A bacterial two-hybrid system further indicated that Rv3789 interacts in vivo with the galactosyltransferase that initiates the elongation of the galactan domain of AG. Biochemical and genetic evidence is thus consistent with Rv3789 belonging to an AG biosynthetic complex, where its role is to reorient DPA to the periplasm, allowing this arabinose donor to then be used in the buildup of the arabinan domains of AG and LAM.

Published

2012

26. Pyrimidine salvage pathway in Mycobacterium tuberculosis.

Author

Villela AD, Sánchez-Quitian ZA, Ducati RG, Santos DS, and Basso LA

Subjects

Cytidine Deaminase metabolism, Mycobacterium tuberculosis metabolism, Nucleoside-Diphosphate Kinase metabolism, Nucleoside-Phosphate Kinase metabolism, Nucleotide Deaminases metabolism, Pentosyltransferases metabolism, Pyrimidine Phosphorylases metabolism, Pyrophosphatases metabolism, Thymidylate Synthase metabolism, Mycobacterium tuberculosis enzymology, Pyrimidines metabolism

Abstract

The causative agent of tuberculosis (TB), Mycobacterium tuberculosis, infects one-third of the world population. TB remains the leading cause of mortality due to a single bacterial pathogen. The worldwide increase in incidence of M. tuberculosis has been attributed to the high proliferation rates of multi and extensively drug-resistant strains, and to co-infection with the human immunodeficiency virus. There is thus a continuous requirement for studies on mycobacterial metabolism to identify promising targets for the development of new agents to combat TB. Singular characteristics of this pathogen, such as functional and structural features of enzymes involved in fundamental metabolic pathways, can be evaluated to identify possible targets for drug development. Enzymes involved in the pyrimidine salvage pathway might be attractive targets for rational drug design against TB, since this pathway is vital for all bacterial cells, and is composed of enzymes considerably different from those present in humans. Moreover, the enzymes of the pyrimidine salvage pathway might have an important role in the mycobacterial latent state, since M. tuberculosis has to recycle bases and/or nucleosides to survive in the hostile environment imposed by the host. The present review describes the enzymes of M. tuberculosis pyrimidine salvage pathway as attractive targets for the development of new antimycobacterial agents. Enzyme functional and structural data have been included to provide a broader knowledge on which to base the search for compounds with selective biological activity.

Published

2011