Your search keyword '"Garrett C. Moraski"' showing total 57 results

1. Dual inhibition of the terminal oxidases eradicates antibiotic‐tolerant Mycobacterium tuberculosis

Author

Bei Shi Lee, Kiel Hards, Curtis A Engelhart, Erik J Hasenoehrl, Nitin P Kalia, Jared S Mackenzie, Ekaterina Sviriaeva, Shi Min Sherilyn Chong, Malathy Sony S Manimekalai, Vanessa H Koh, John Chan, Jiayong Xu, Sylvie Alonso, Marvin J Miller, Adrie J C Steyn, Gerhard Grüber, Dirk Schnappinger, Michael Berney, Gregory M Cook, Garrett C Moraski, and Kevin Pethe

Subjects

antibiotic‐tolerance, cytochrome bcc‐aa3, cytochrome bd oxidase, oxidative phosphorylation, Q203, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract The approval of bedaquiline has placed energy metabolism in the limelight as an attractive target space for tuberculosis antibiotic development. While bedaquiline inhibits the mycobacterial F1F0 ATP synthase, small molecules targeting other components of the oxidative phosphorylation pathway have been identified. Of particular interest is Telacebec (Q203), a phase 2 drug candidate inhibitor of the cytochrome bcc:aa3 terminal oxidase. A functional redundancy between the cytochrome bcc:aa3 and the cytochrome bd oxidase protects M. tuberculosis from Q203‐induced death, highlighting the attractiveness of the bd‐type terminal oxidase for drug development. Here, we employed a facile whole‐cell screen approach to identify the cytochrome bd inhibitor ND‐011992. Although ND‐011992 is ineffective on its own, it inhibits respiration and ATP homeostasis in combination with Q203. The drug combination was bactericidal against replicating and antibiotic‐tolerant, non‐replicating mycobacteria, and increased efficacy relative to that of a single drug in a mouse model. These findings suggest that a cytochrome bd oxidase inhibitor will add value to a drug combination targeting oxidative phosphorylation for tuberculosis treatment.

Published

2020

2. Targeting the Mycobacterium ulcerans cytochrome bc 1 :aa 3 for the treatment of Buruli ulcer

Author

Nicole Scherr, Raphael Bieri, Sangeeta S. Thomas, Aurélie Chauffour, Nitin Pal Kalia, Paul Schneide, Marie-Thérèse Ruf, Araceli Lamelas, Malathy S. S. Manimekalai, Gerhard Grüber, Norihisa Ishii, Koichi Suzuki, Marcel Tanner, Garrett C. Moraski, Marvin J. Miller, Matthias Witschel, Vincent Jarlier, Gerd Pluschke, and Kevin Pethe

Subjects

Science

Abstract

Mycobacterium ulcerans is the causative agent of Buruli ulcer (BU). Existing anti-tubercular drugs have been used to treat the condition with varying success. Here, the authors show that a clinical-stage drug candidate for tuberculosis, Q203, is effective at killing M. ulcerans and is a promising therapeutic candidate for BU.

Published

2018

3. Syntheses and Structure–Activity Relationships of N-Phenethyl-Quinazolin-4-yl-Amines as Potent Inhibitors of Cytochrome bd Oxidase in Mycobacterium tuberculosis

Author

Sarah M. Hopfner, Bei Shi Lee, Nitin P. Kalia, Marvin J. Miller, Kevin Pethe, and Garrett C. Moraski

Subjects

tuberculosis, drug development, structure–activity relationships, quinazoline, energy metabolism, cytochrome bd oxidase, Technology, Engineering (General). Civil engineering (General), TA1-2040, Biology (General), QH301-705.5, Physics, QC1-999, Chemistry, QD1-999

Abstract

The development of cytochrome bd oxidase (cyt-bd) inhibitors are needed for comprehensive termination of energy production in Mycobacterium tuberculosis (Mtb) to treat tuberculosis infections. Herein, we report on the structure-activity-relationships (SAR) of 22 new N-phenethyl-quinazolin-4-yl-amines that target cyt-bd. Our focused set of compounds was synthesized and screened against three mycobacterial strains: Mycobacterium bovis BCG, Mycobacterium tuberculosis H37Rv and the clinical isolate Mycobacterium tuberculosis N0145 with and without the cytochrome bcc:aa3 inhibitor Q203 in an ATP depletion assay. Two compounds, 12a and 19a, were more active against all three strains than the naturally derived cyt-bd inhibitor aurachin D.

Published

2021

4. Intracellular and in vivo evaluation of imidazo[2,1-b]thiazole-5-carboxamide anti-tuberculosis compounds.

Author

Garrett C Moraski, Nathalie Deboosère, Kate L Marshall, Heath A Weaver, Alexandre Vandeputte, Courtney Hastings, Lisa Woolhiser, Anne J Lenaerts, Priscille Brodin, and Marvin J Miller

Subjects

Medicine, Science

Abstract

The imidazo[2,1-b]thiazole-5-carboxamides (ITAs) are a promising class of anti-tuberculosis agents shown to have potent activity in vitro and to target QcrB, a key component of the mycobacterial cytochrome bcc-aa3 super complex critical for the electron transport chain. Herein we report the intracellular macrophage potency of nine diverse ITA analogs with MIC values ranging from 0.0625-2.5 μM and mono-drug resistant potency ranging from 0.0017 to 7 μM. The in vitro ADME properties (protein binding, CaCo-2, human microsomal stability and CYP450 inhibition) were determined for an outstanding compound of the series, ND-11543. ND-11543 was tolerable at >500 mg/kg in mice and at a dose of 200 mg/kg displayed good drug exposure in mice with an AUC(0-24h) >11,700 ng·hr/mL and a >24 hr half-life. Consistent with the phenotype observed with other QcrB inhibitors, compound ND-11543 showed efficacy in a chronic murine TB infection model when dosed at 200 mg/kg for 4 weeks. The efficacy was not dependent upon exposure, as pre-treatment with a known CYP450-inhibitor did not substantially improve efficacy. The ITAs are an interesting scaffold for the development of new anti-TB drugs especially in combination therapy based on their favorable properties and novel mechanism of action.

Published

2020

5. Hydride-induced Meisenheimer complex formation reflects activity of nitro aromatic anti-tuberculosis compounds

Author

Kevin Pethe, Karin Savková, Lowell D. Markley, Marvin J. Miller, Rui Ma, Gauri Shetye, Garrett C. Moraski, Bei Shi Lee, Katarína Mikušová, Patricia A. Miller, Rui Liu, and Scott G. Franzblau

Subjects

Pharmacology, chemistry.chemical_classification, 0303 health sciences, 010405 organic chemistry, Chemistry, Hydride, Organic Chemistry, Pharmaceutical Science, 01 natural sciences, Biochemistry, Medicinal chemistry, Meisenheimer complex, 0104 chemical sciences, 03 medical and health sciences, Enzyme, Anti tuberculosis, Drug Discovery, Nitro, Molecular Medicine, 030304 developmental biology

Abstract

The formation efficiency of hydride-induced Meisenheimer complexes of nitroaromatic compounds is consistent with their anti-TB activities exemplied by MDL860 and benzothiazol N-oxide (BTO) analogs. Herein we report that nitro cyano phenoxybenzenes (MDL860 and analogs) reacted slowly and incompletely which reflected their moderate anti-TB activity, in contrast to the instantaneous reaction of BTO derivatives to quantitatively generate Meisenheimer complexes which corresponded to their enhanced anti-TB activity. These results were corroborated by mycobacterial and radiolabelling studies that confirmed inhibition of the DprE1 enzyme by BTO derivatives but not MDL860 analogs.

Published

2021

6. Bactericidal activity of an imidazo[1, 2-a]pyridine using a mouse M. tuberculosis infection model.

Author

Yong Cheng, Garrett C Moraski, Jeffrey Cramer, Marvin J Miller, and Jeffrey S Schorey

Subjects

Medicine, Science

Abstract

Tuberculosis remains a global threat due in part to the long treatment regimen and the increased prevalence of drug resistant M. tuberculosis strains. Therefore, new drug regimens are urgently required to combat this deadly disease. We previously synthesized and evaluated a series of new anti-tuberculosis compounds which belong to the family of imidazo[1,2-a]pyridines. This family of compounds showed low nM MIC (minimal inhibitory concentration) values against M. tuberculosis in vitro. In this study, a derivative of imidazo[1,2-a]pyridines, (N-(4-(4-chlorophenoxy)benzyl)-2,7-dimethylimidazo[1,2-a]pyridine-3-carboxamide) (ND-09759), was selected as a promising lead compound to determine its protective efficacy using a mouse infection model. Pharmacokinetic analysis of ND-09759 determined that at a dosage of 30 mg/kg mouse body weight (PO) gave a maximum serum drug concentration (Cmax) of 2.9 µg/ml and a half-life of 20.1 h. M. tuberculosis burden in the lungs and spleens was significantly decreased in mice treated once daily 6 days per week for 4-weeks with ND-09759 compared to untreated mice and this antibiotic activity was equivalent to isoniazid (INH) and rifampicin (RMP), two first-line anti-TB drugs. We observed slightly higher efficacy when using a combination of ND-09759 with either INH or RMP. Finally, the histopathological analysis revealed that infected mice treated with ND-09759 had significantly reduced inflammation relative to untreated mice. In conclusion, our findings indicate ND-09759 might be a potent candidate for the treatment of active TB in combination with current standard anti-TB drugs.

Published

2014

7. Structure guided generation of thieno[3,2-d]pyrimidin-4-amine Mycobacterium tuberculosis bd oxidase inhibitors

Author

Marvin J. Miller, Kevin Pethe, Bei Shi Lee, Sarah M. Hopfner, Garrett C. Moraski, and Nitin Pal Kalia

Subjects

0301 basic medicine, Tuberculosis, Cytochrome, 030106 microbiology, Pharmaceutical Science, Context (language use), Biochemistry, Mycobacterium tuberculosis, 03 medical and health sciences, Drug Discovery, medicine, IC50, Pharmacology, Mycobacterium bovis, Oxidase test, Strain (chemistry), biology, Chemistry, Organic Chemistry, medicine.disease, biology.organism_classification, Molecular biology, 030104 developmental biology, biology.protein, Molecular Medicine

Abstract

Cytochrome bd oxidase (Cyt-bd) is an attractive drug target in Mycobacterium tuberculosis, especially in the context of developing a drug combination targeting energy metabolism. However, currently few synthetically assessable scaffolds target Cyt-bd. Herein, we report that thieno[3,2-d]pyrimidin-4-amines inhibit Cyt-bd, and report an initial structure–activity-relationship (SAR) of 13 compounds in three mycobacterial strains: Mycobacterium bovis BCG, Mycobacterium tuberculosis H37Rv and Mycobacterium tuberculosis clinical isolate N0145 in an established ATP depletion assay with or without the cytochrome bcc : aa(3) (QcrB) inhibitor Q203. All compounds displayed activity against M. bovis BCG and the M. tuberculosis clinical isolate strain N0145 with ATP IC(50) values from 6 to 54 μM in the presence of Q203 only, as expected from a Cyt-bd inhibitor. All derivatives were much less potent against M. tuberculosis H37Rv compared to N0145 (IC(50)'s from 24 to >100 μM and 9–52 μM, respectively), an observation that may be attributed to the higher expression of the Cyt-bd-encoding genes in the laboratory-adapted M. tuberculosis H37Rv strain. N-(4-(tert-butyl)phenethyl)thieno[3,2-d]pyrimidin-4-amine (19) was the most active compound with ATP IC(50) values from 6 to 18 μM against all strains in the presence of Q203, making it a good chemical probe for interrogation the function of the mycobacterial Cyt-bd under various physiological conditions.

Published

2021

8. A dual read-out assay to evaluate the potency of compounds active against Mycobacterium tuberculosis.

Author

Juliane Ollinger, Mai Ann Bailey, Garrett C Moraski, Allen Casey, Stephanie Florio, Torey Alling, Marvin J Miller, and Tanya Parish

Subjects

Medicine, Science

Abstract

Tuberculosis is a serious global health problem caused by the bacterium Mycobacterium tuberculosis. There is an urgent need for discovery and development of new treatments, but this can only be accomplished through rapid and reproducible M. tuberculosis assays designed to identify potent inhibitors. We developed an automated 96-well assay utilizing a recombinant strain of M. tuberculosis expressing a far-red fluorescent reporter to determine the activity of novel compounds; this allowed us to measure growth by monitoring both optical density and fluorescence. We determined that optical density and fluorescence were correlated with cell number during logarithmic phase growth. Fluorescence was stably maintained without antibiotic selection over 5 days, during which time cells remained actively growing. We optimized parameters for the assay, with the final format being 5 days' growth in 96-well plates in the presence of 2% w/v DMSO. We confirmed reproducibility using rifampicin and other antibiotics. The dual detection method allows for a reproducible calculation of the minimum inhibitory concentration (MIC), at the same time detecting artefacts such as fluorescence quenching or compound precipitation. We used our assay to confirm anti-tubercular activity and establish the structure activity relationship (SAR) around the imidazo[1,2-a]pyridine-3-carboxamides, a promising series of M. tuberculosis inhibitors.

Published

2013

9. Decarboxylation involving a ferryl, propionate, and a tyrosyl group in a radical relay yields heme b

Author

Bennett R. Streit, Eric M. Shepard, Jennifer L. DuBois, Garrett C. Moraski, Krista A. Shisler, Arianna I. Celis, Gudrun S. Lukat-Rodgers, and Kenton R. Rodgers

Subjects

Models, Molecular, 0301 basic medicine, Reaction mechanism, Free Radicals, Carboxy-Lyases, Decarboxylation, Heme, Crystallography, X-Ray, 010402 general chemistry, Ferric Compounds, 01 natural sciences, Biochemistry, Medicinal chemistry, Catalysis, 03 medical and health sciences, chemistry.chemical_compound, Reaction rate constant, Catalytic Domain, Kinetic isotope effect, Propionates, Molecular Biology, Oxidative decarboxylation, chemistry.chemical_classification, Electron Spin Resonance Spectroscopy, Hydrogen Peroxide, Cell Biology, 0104 chemical sciences, Kinetics, Heme B, 030104 developmental biology, chemistry, Mutation, Enzymology, Propionate, Tyrosine, Oxidation-Reduction

Abstract

The H(2)O(2)-dependent oxidative decarboxylation of coproheme III is the final step in the biosynthesis of heme b in many microbes. However, the coproheme decarboxylase reaction mechanism is unclear. The structure of the decarboxylase in complex with coproheme III suggested that the substrate iron, reactive propionates, and an active-site tyrosine convey a net 2e(−)/2H(+) from each propionate to an activated form of H(2)O(2). Time-resolved EPR spectroscopy revealed that Tyr-145 formed a radical species within 30 s of the reaction of the enzyme–coproheme complex with H(2)O(2). This radical disappeared over the next 270 s, consistent with a catalytic intermediate. Use of the harderoheme III intermediate as substrate or substitutions of redox-active side chains (W198F, W157F, or Y113S) did not strongly affect the appearance or intensity of the radical spectrum measured 30 s after initiating the reaction with H(2)O(2), nor did it change the ∼270 s required for the radical signal to recede to ≤10% of its initial intensity. These results suggested Tyr-145 as the site of a catalytic radical involved in decarboxylating both propionates. Tyr-145(•) was accompanied by partial loss of the initially present Fe(III) EPR signal intensity, consistent with the possible formation of Fe(IV)=O. Site-specifically deuterated coproheme gave rise to a kinetic isotope effect of ∼2 on the decarboxylation rate constant, indicating that cleavage of the propionate Cβ–H bond was partly rate-limiting. The inferred mechanism requires two consecutive hydrogen atom transfers, first from Tyr-145 to the substrate Fe/H(2)O(2) intermediate and then from the propionate Cβ–H to Tyr-145(•).

Published

2018

10. Structure-Based Mechanism for Oxidative Decarboxylation Reactions Mediated by Amino Acids and Heme Propionates in Coproheme Decarboxylase (HemQ)

Author

Gudrun S. Lukat-Rodgers, Bennett R. Streit, George H. Gauss, Kenton R. Rodgers, Krista A. Shisler, Arianna I. Celis, John W. Peters, Garrett C. Moraski, and Jennifer L. DuBois

Subjects

0301 basic medicine, Carboxy-Lyases, Stereochemistry, Substrate analog, Decarboxylation, Biochemistry, Article, Catalysis, Cofactor, Geobacillus stearothermophilus, 03 medical and health sciences, chemistry.chemical_compound, Colloid and Surface Chemistry, Organic chemistry, Amino Acids, Heme, Oxidative decarboxylation, Bond cleavage, chemistry.chemical_classification, Molecular Structure, 030102 biochemistry & molecular biology, biology, General Chemistry, Amino acid, Kinetics, Heme B, 030104 developmental biology, chemistry, Propionate, biology.protein, Oxidation-Reduction

Abstract

Coproheme decarboxylase catalyzes two sequential oxidative decarboxylations with H2O2 as the oxidant, coproheme III as substrate and cofactor, and heme b as the product. Each reaction breaks a C-C bond and results in net loss of hydride, via steps that are not clear. Solution and solid-state structural characterization of the protein in complex with a substrate analog revealed a highly unconventional H2O2-activating distal environment with the reactive propionic acids (2 and 4) on the opposite side of the porphyrin plane. This suggested that, in contrast to direct C-H bond cleavage catalyzed by a high-valent iron intermediate, the coproheme oxidations must occur through mediating amino acid residues. A tyrosine that hydrogen bonds to propionate 2 in a position analogous to the substrate in ascorbate peroxidase is essential for both decarboxylations, while a lysine that salt bridges to propionate 4 is required solely for the second. A mechanism is proposed in which propionate 2 relays an oxidizing equivalent from a coproheme compound I intermediate to the reactive deprotonated tyrosine, forming Tyr■. This residue then abstracts a net hydrogen atom (H■) from propionate 2, followed by migration of the unpaired propionyl electron to the coproheme iron to yield the ferric harderoheme and CO2 products. A similar pathway is proposed for decarboxylation of propionate 4, but with a lysine residue as an essential proton shuttle. The proposed reaction suggests an extended relay of heme-mediated e−/H+ transfers and a novel route for the conversion of carboxylic acids to alkenes.

Published

2017

11. Imidazo[1,2- a ]Pyridine-3-Carboxamides Are Active Antimicrobial Agents against Mycobacterium avium Infection In Vivo

Author

Jeffery S. Schorey, Marvin J. Miller, Sang-Hyun Cho, Garrett C. Moraski, Scott G. Franzblau, Thierry Masquelin, Yong Cheng, Jeffrey W Cramer, and Godfrey Alexander Glenn

Subjects

0301 basic medicine, Pyridines, medicine.drug_class, 030106 microbiology, Mycobacterium avium-intracellulare infection, Mycobacterium Avium Infection, Antibiotics, Spleen, Microbial Sensitivity Tests, Microbiology, Mice, 03 medical and health sciences, Anti-Infective Agents, In vivo, medicine, Animals, Pharmacology (medical), Mechanisms of Action: Physiological Effects, Mycobacterium avium-intracellulare Infection, Pharmacology, biology, business.industry, Imidazoles, Antimicrobial, medicine.disease, biology.organism_classification, Regimen, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, business, Mycobacterium avium, Mycobacterium

Abstract

A panel of six imidazo[1,2- a ]pyridine-3-carboxamides (IAPs) were shown to have low-micromolar activity against Mycobacterium avium strains. Compound ND-10885 (compound 2) showed significant activity in the lung, spleen, and liver in a mouse M. avium infection model. A combined regimen consisting of ND-10885 (compound 2) and rifampin was additive in its anti- M. avium activity in the lung. Our data indicate that IAPs represent a new class of antibiotics that are active against M. avium and could potentially serve as an effective addition to a combined treatment regimen.

Published

2016

12. Carbon metabolism modulates the efficacy of drugs targeting the cytochrome bc1:aa3 in Mycobacterium tuberculosis

Author

Bei Shi Lee, Nurlilah Binte Ab Rahman, Garrett C. Moraski, Nitin Pal Kalia, Marvin J. Miller, Kevin Pethe, School of Biological Sciences, and Lee Kong Chian School of Medicine (LKCMedicine)

Subjects

0301 basic medicine, Bioenergetics, Cytochrome, lcsh:Medicine, Oxidative phosphorylation, Mycobacterium tuberculosis, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Chemistry [Science], Potency, Tuberculosis, lcsh:Science, Oxidase test, Multidisciplinary, biology, Chemistry, Cytochrome bc1, Antimicrobials, lcsh:R, biology.organism_classification, 3. Good health, 030104 developmental biology, Biochemistry, biology.protein, lcsh:Q, 030217 neurology & neurosurgery

Abstract

The influence of carbon metabolism on oxidative phosphorylation is poorly understood in mycobacteria. M. tuberculosis expresses two respiratory terminal oxidases, the cytochrome bc1:aa3 and the cytochrome bd oxidase, which are jointly required for oxidative phosphorylation and mycobacterial viability. The essentiality of the cytochrome bc1:aa3 for optimum growth is illustrated by its vulnerability to chemical inhibition by the clinical drug candidate Q203 and several other chemical series. The cytochrome bd oxidase is not strictly essential for growth but is required to maintain bioenergetics when the function of the cytochrome bc1:aa3 is compromised. In this study, we observed that the potency of drugs targeting the cytochrome bc1:aa3 is influenced by carbon metabolism. The efficacy of Q203 and related derivatives was alleviated by glycerol supplementation. The negative effect of glycerol supplementation on Q203 potency correlated with an upregulation of the cytochrome bd oxidase-encoding cydABDC operon. Upon deletion of cydAB, the detrimental effect of glycerol on the potency of Q203 was abrogated. The same phenomenon was also observed in recent clinical isolates, but to a lesser extent compared to the laboratory-adapted strain H37Rv. This study reinforces the importance of optimizing in vitro culture conditions for drug evaluation in mycobacteria, a factor which appeared to be particularly essential for drugs targeting the cytochrome bc1:aa3 terminal oxidase.

Published

2019

13. Carbon metabolism modulates the efficacy of drugs targeting the cytochrome bc

Author

Nitin P, Kalia, Bei, Shi Lee, Nurlilah B, Ab Rahman, Garrett C, Moraski, Marvin J, Miller, and Kevin, Pethe

Subjects

Glycerol, Pyridines, Antimicrobials, Antitubercular Agents, Drug Resistance, Imidazoles, Gene Expression Regulation, Bacterial, Mycobacterium tuberculosis, Carbon, Article, Electron Transport Complex IV, Electron Transport Complex III, Piperidines, Mutation, Operon, Tuberculosis, Gene Deletion

Abstract

The influence of carbon metabolism on oxidative phosphorylation is poorly understood in mycobacteria. M. tuberculosis expresses two respiratory terminal oxidases, the cytochrome bc1:aa3 and the cytochrome bd oxidase, which are jointly required for oxidative phosphorylation and mycobacterial viability. The essentiality of the cytochrome bc1:aa3 for optimum growth is illustrated by its vulnerability to chemical inhibition by the clinical drug candidate Q203 and several other chemical series. The cytochrome bd oxidase is not strictly essential for growth but is required to maintain bioenergetics when the function of the cytochrome bc1:aa3 is compromised. In this study, we observed that the potency of drugs targeting the cytochrome bc1:aa3 is influenced by carbon metabolism. The efficacy of Q203 and related derivatives was alleviated by glycerol supplementation. The negative effect of glycerol supplementation on Q203 potency correlated with an upregulation of the cytochrome bd oxidase-encoding cydABDC operon. Upon deletion of cydAB, the detrimental effect of glycerol on the potency of Q203 was abrogated. The same phenomenon was also observed in recent clinical isolates, but to a lesser extent compared to the laboratory-adapted strain H37Rv. This study reinforces the importance of optimizing in vitro culture conditions for drug evaluation in mycobacteria, a factor which appeared to be particularly essential for drugs targeting the cytochrome bc1:aa3 terminal oxidase.

Published

2018

14. PvdF of pyoverdin biosynthesis is a structurally unique N

Author

Nikola, Kenjić, Matthew R, Hoag, Garrett C, Moraski, Carol A, Caperelli, Graham R, Moran, and Audrey L, Lamb

Subjects

Hydroxymethyl and Formyl Transferases, Models, Molecular, Folic Acid, Protein Conformation, Pseudomonas aeruginosa, Oligopeptides, Article, Formyltetrahydrofolates

Abstract

The hydroxyornithine transformylase from Pseudomonas aeruginosa is known by the gene name pvdF, and has been hypothesized to use N(10)-formyltetrahydrofolate (N(10)-fTHF) as a co-substrate formyl donor to convert N(5)-hydroxyornithine (OHOrn) to N(5)-formyl- N(5)-hydroxyornithine (fOHOrn). PvdF is in the biosynthetic pathway for pyoverdin biosynthesis, a siderophore generated under iron-limiting conditions that has been linked to virulence, quorum sensing and biofilm formation. The structure of PvdF was determined by X-ray crystallography to 2.3 Å, revealing a formyltransferase fold consistent with N(10)-formyltetrahydrofolate dependent enzymes, such as the glycinamide ribonucleotide transformylases, N-sugar transformylases and methionyl-tRNA transformylases. Whereas the core structure, including the catalytic triad, is conserved, PvdF has three insertions of 18 or more amino acids, which we hypothesize are key to binding the OHOrn substrate. Steady state kinetics revealed a non-hyperbolic rate curve, promoting the hypothesis that PvdF uses a random-sequential mechanism, and favors folate binding over OHOrn.

Published

2018

15. Imidazopyridine Compounds Inhibit Mycobacterial Growth by Depleting ATP Levels

Author

Thierry Masquelin, Julie V. Early, Garrett C. Moraski, Philip Arthur Hipskind, Marvin J. Miller, Tanya Parish, Heather Wescott, Torey Alling, Theresa O’Malley, and Anuradha Kumar

Subjects

0301 basic medicine, Imidazopyridine, mycobacteria, Pyridines, 030106 microbiology, Hypothetical protein, Mutant, Antitubercular Agents, Microbial Sensitivity Tests, medicine.disease_cause, antibiotics, mycobacterium, drug discovery, Electron Transport Complex IV, 03 medical and health sciences, Adenosine Triphosphate, Mechanisms of Resistance, medicine, Cytochrome c oxidase, Pharmacology (medical), Mode of action, Pharmacology, Mutation, drug resistance, biology, Whole Genome Sequencing, Chemistry, Imidazoles, cytochrome oxidase, Mycobacterium tuberculosis, biology.organism_classification, In vitro, 3. Good health, ATP, antibacterial, Infectious Diseases, Biochemistry, biology.protein, Bacteria, respiration

Abstract

The imidazopyridines are a promising new class of antitubercular agents with potent activity in vitro and in vivo . We isolated mutants of Mycobacterium tuberculosis resistant to a representative imidazopyridine; the mutants had large shifts (>20-fold) in MIC. Whole-genome sequencing revealed mutations in Rv1339, a hypothetical protein of unknown function. We isolated mutants resistant to three further compounds from the series; resistant mutants isolated from two of the compounds had single nucleotide polymorphisms in Rv1339 and resistant mutants isolated from the third compound had single nucleotide polymorphisms in QcrB, the proposed target for the series. All the strains were resistant to two compounds, regardless of the mutation, and a strain carrying the QcrB T313I mutation was resistant to all of the imidazopyridine derivatives tested, confirming cross-resistance. By monitoring pH homeostasis and ATP generation, we confirmed that compounds from the series were targeting QcrB; imidazopyridines disrupted pH homeostasis and depleted ATP, providing further evidence of an effect on the electron transport chain. A representative compound was bacteriostatic against replicating bacteria, consistent with a mode of action against QcrB. The series had a narrow inhibitory spectrum, with no activity against other bacterial species. No synergy or antagonism was seen with other antituberculosis drugs under development. In conclusion, our data support the hypothesis that the imidazopyridine series functions by reducing ATP generation via inhibition of QcrB.

Published

2018

16. Unusual Peroxide-Dependent, Heme-Transforming Reaction Catalyzed by HemQ

Author

Garrett C. Moraski, Jennifer L. DuBois, Gudrun S. Lukat-Rodgers, Arianna I. Celis, Timothy D. Lash, Ravi Kant, Bennett R. Streit, and Kenton R. Rodgers

Subjects

Models, Molecular, Staphylococcus aureus, Chemistry, Decarboxylation, Heme, Hydrogen Peroxide, Biochemistry, Medicinal chemistry, Peroxide, Article, Catalysis, Kinetics, chemistry.chemical_compound, Heme B, Bacterial Proteins, Peracetic acid, Yield (chemistry), Organic chemistry, Peracetic Acid, Oxidoreductases, Propionates

Abstract

A recently proposed pathway for heme b biosynthesis, common to diverse bacteria, has the conversion of two of the four propionates on coproheme III to vinyl groups as its final step. This reaction is catalyzed in a cofactor-independent, H2O2-dependent manner by the enzyme HemQ. Using the HemQ from Staphylococcus aureus (SaHemQ), the initial decarboxylation step was observed to rapidly and obligately yield the three-propionate harderoheme isomer III as the intermediate, while the slower second decarboxylation appeared to control the overall rate. Both synthetic harderoheme isomers III and IV reacted when bound to HemQ, the former more slowly than the latter. While H2O2 is the assumed biological oxidant, either H2O2 or peracetic acid yielded the same intermediates and products, though amounts significantly greater than the expected 2 equiv were required in both cases and peracetic acid reacted faster. The ability of peracetic acid to substitute for H2O2 suggests that, despite the lack of catalytic residues conventionally present in heme peroxidase active sites, reaction pathways involving high-valent iron intermediates cannot be ruled out.

Published

2015

17. Putting Tuberculosis (TB) To Rest: Transformation of the Sleep Aid, Ambien, and 'Anagrams' Generated Potent Antituberculosis Agents

Author

Garrett C. Moraski, Jeffrey R. Anderson, Scott G. Franzblau, Surafel Mulugeta, Patricia A. Miller, Sang-Hyun Cho, Marvin J. Miller, Tanya Parish, Juliane Ollinger, Helena I. Boshoff, and Mai A. Bailey

Subjects

Zolpidem, Letter, Tuberculosis, anti-TB, Pharmacology, 01 natural sciences, Mycobacterium tuberculosis, 03 medical and health sciences, Anagrams, medicine, Potency, Uncategorized, 030304 developmental biology, 0303 health sciences, biology, 010405 organic chemistry, Chemistry, imidazopyridine analogues, Rational design, biology.organism_classification, medicine.disease, 3. Good health, 0104 chemical sciences, Infectious Diseases, tuberculosis, Ambien, zolpidem, medicine.drug

Abstract

Zolpidem (Ambien, 1) is an imidazo[1,2-a]pyridine-3-acetamide and an approved drug for the treatment of insomnia. As medicinal chemists enamored by how structure imparts biological function, we found it to have strikingly similar structure to the antitubercular imidazo[1,2-a]pyridine-3-carboxyamides. Zolpidem was found to have antituberculosis activity (MIC of 10-50 ��M) when screened against replicating Mycobacterium tuberculosis (Mtb) H37Rv. Manipulation of the Zolpidem structure, notably, to structural isomers ("anagrams"), attains remarkably improved potency (5, MIC of 0.004 ��M) and impressive potency against clinically relevant drug-sensitive, multi- and extensively drug-resistant Mtb strains (MIC < 0.03 ��M). Zolpidem anagrams and analogues were synthesized and evaluated for their antitubercular potency, toxicity, and spectrum of activity against nontubercular mycobacteria and Gram-positive and Gram-negative bacteria. These efforts toward the rational design of isomeric anagrams of a well-known sleep aid underscore the possibility that further optimization of the imidazo[1,2-a]pyridine core may well "put TB to rest".

Published

2015

18. Preparation and Evaluation of Potent Pentafluorosulfanyl Substituted Anti-Tuberculosis Compounds

Author

Patricia S. Tsang, Helena I. Boshoff, Garrett C. Moraski, Marvin J. Miller, Ryan Bristol, and Natalie Seeger

Subjects

0301 basic medicine, Tuberculosis, Pyridines, Antitubercular Agents, Sulfanilic Acids, Drug resistance, Plasma protein binding, Microbial Sensitivity Tests, Pharmacology, Biochemistry, Article, Cell Line, Mycobacterium tuberculosis, 03 medical and health sciences, Structure-Activity Relationship, Anti tuberculosis, Drug Discovery, Drug Resistance, Bacterial, medicine, Potency, Animals, Humans, General Pharmacology, Toxicology and Pharmaceutics, ADME, biology, Chemistry, Organic Chemistry, Imidazoles, medicine.disease, biology.organism_classification, 030104 developmental biology, Microsome, Molecular Medicine

Abstract

The global fight to stop tuberculosis (TB) remains a great challenge, particularly with the increase in drug resistant strains and a lack of funding to support the development of new treatments. To bolster a precarious drug pipeline, we have prepared a focused panel of eight pentafluorosulfanyl (SF5) compounds (13 – 20) which were screened for their activity against Mycobacterium tuberculosis (Mtb) H37Rv in three different assay conditions and media. All eight compounds had sub-micromolar potency and four (13, 15, 16, and 19) displayed MICs

Published

2017

19. Scaffold-switching: An exploration of 5,6-fused bicyclic heteroaromatics systems to afford antituberculosis activity akin to the imidazo[1,2-a]pyridine-3-carboxylates

Author

Scott G. Franzblau, Allen G. Oliver, Lowell D. Markley, Sang-Hyun Cho, Garrett C. Moraski, and Marvin J. Miller

Subjects

Pyrimidine, Pyridines, Stereochemistry, Clinical Biochemistry, Antitubercular Agents, Pharmaceutical Science, Microbial Sensitivity Tests, Hydrocarbons, Aromatic, Biochemistry, Article, Mycobacterium tuberculosis, Bridged Bicyclo Compounds, Structure-Activity Relationship, chemistry.chemical_compound, Heterocyclic Compounds, Drug Discovery, Structure–activity relationship, Candida albicans, Molecular Biology, Mycobacterium kansasii, Mycobacterium bovis, Dose-Response Relationship, Drug, Molecular Structure, biology, Bicyclic molecule, Organic Chemistry, Imidazoles, biology.organism_classification, Pyrimidines, chemistry, Molecular Medicine, Mycobacterium

Abstract

A set of 5,6-fused bicyclic heteroaromatic scaffolds were investigated for their in vitro anti-tubercular activity versus replicating and non-replicating strains of Mycobacterium tuberculosis (Mtb) in an attempt to find an alternative scaffold to the imidazo[1,2-a]pyridine and imidazo[1,2-a]pyrimidines that were previously shown to have potent activity against replicating and drug resistant Mtb. The five new bicyclic heteroaromatic scaffolds explored in this study include a 2,6-dimethylimidazo[1,2-b]pyridazine-3-carboxamide (7), a 2,6-dimethyl-1H-indole-3-carboxamide (8), a 6-methyl-1H-indazole-3-carboxamide (9), a 7-methyl-[1,2,4]triazolo[4,3-a]pyridine-3-carboxamide (10), and a 5,7-dimethyl-[1,2,4]triazolo[1,5-a]pyrimidine-2-carboxamide (11). Additionally, imidazo[1,2-a]pyridines isomers (2 and 12) and a homologous imidazo[1,2-a]pyrimidine isomer (6) were prepared and compared. Compounds 2 and 6 were found to be the most potent against H37Rv Mtb (MIC’s of 0.1 μM and 1.3 μM) and were inactive (MIC >128 μM) against Staphylococcus aureus, Escherichia coli and Candida albicans. Against other non-tubercular mycobacteria strains, compounds 2 and 6 had activity against Mycobacterium avium (16 and 122 μM, respectively), Mycobacterium kansasii (4 and 19 μM, respectively), Mycobacterium bovis BCG (1 and 8 μM, respectively) while all the other scaffolds were inactive (>128 μM).

Published

2014

20. Advancement of Imidazo[1,2-a]pyridines with Improved Pharmacokinetics and nM Activity vs. Mycobacterium tuberculosis

Author

Jeffrey W Cramer, Mai A. Bailey, Helena I. Boshoff, Garrett C. Moraski, Marvin J. Miller, Lowell D. Markley, Philip Arthur Hipskind, Torey Alling, Juliane Ollinger, and Tanya Parish

Subjects

biology, business.industry, Organic Chemistry, Male mice, Drug resistance, Pharmacology, biology.organism_classification, Biochemistry, Mycobacterium tuberculosis, Pharmacokinetics, Mic values, Drug Discovery, Mycobacterium tuberculosis H37Rv, Medicine, Potency, business, Bacteria

Abstract

A set of 14 imidazo[1,2-a]pyridine-3-carboxamides was synthesized and screened against Mycobacterium tuberculosis H37Rv. The minimum inhibitory concentrations of 12 of these agents were ≤1 μM against replicating bacteria and 5 compounds (9, 12, 16, 17, and 18) had MIC values ≤0.006 μM. Compounds 13 and 18 were screened against a panel of MDR and XDR drug resistant clinical Mtb strains with the potency of 18 surpassing that of clinical candidate PA-824 by nearly 10-fold. The in vivo pharmacokinetics of compounds 13 and 18 were evaluated in male mice by oral (PO) and intravenous (IV) routes. These results indicate that readily synthesized imidazo[1,2-a]pyridine-3-carboxamides are an exciting new class of potent, selective anti-TB agents that merit additional development opportunities.

Published

2013

21. Allylic thiocyanates as a new class of antitubercular agents

Author

Garrett C. Moraski, CH Hwang, Gustavo Pozza Silveira, Scott G. Franzblau, Misael Ferreira, Sang-Hyun Cho, Luciano Fernandes, and Marcus M. Sá

Subjects

Isothiouronium, Allylic rearrangement, Stereochemistry, Clinical Biochemistry, Antitubercular Agents, Pharmaceutical Science, Microbial Sensitivity Tests, Biochemistry, Mycobacterium tuberculosis, chemistry.chemical_compound, Chlorocebus aethiops, Drug Discovery, Animals, Humans, Tuberculosis, Vero Cells, Molecular Biology, Antibacterial agent, Thiocyanate, biology, Aryl, Organic Chemistry, respiratory system, biology.organism_classification, In vitro, Allyl Compounds, chemistry, Vero cell, Molecular Medicine, Thiocyanates

Abstract

TB is a global public health emergency in which new drugs are desperately needed. Herein we report on the synthesis of a diverse panel of 41 aryl allylic azides, thiocyanates, isothiouronium salts, and N,N′-diacetylisothioureas that were evaluated for their in vitro activity against replicating and non-replicating Mycobacterium tuberculosis (Mtb) H37Rv and toxicity to VERO cells. We found a selective group of new and promising compounds having good (micromolar) to excellent (sub-micromolar) potency against replicating Mtb H37Rv. Allylic thiocyanates bearing halophenyl (halo = 2-Br, 4-Br, 4-Cl, 4-F), 4-methylphenyl and 2-naphthyl moieties were the most active as antitubercular agents. In particular, the 2-bromophenyl-substituted thiocyanate showed MIC = 0.25 μM against replicating Mtb, MIC = 8.0 μM against non-replicating Mtb and IC50 = 32 μM in the VERO cellular toxicity assay.

Published

2012

22. Synthesis of Dideoxymycobactin Antigens Presented by CD1a Reveals T Cell Fine Specificity for Natural Lipopeptide Structures

Author

Adam Uzieblo, Dirk M. Zajonc, Tan-Yun Cheng, Yanping Xu, Gregory W. Endres, Garrett C. Moraski, Catherine E. Costello, Jingdan Hu, D. Branch Moody, Marvin J. Miller, Andrew J. Walz, Anne Kasmar, and David C. Young

Subjects

Models, Molecular, Stereochemistry, T-Lymphocytes, T cell, Mycobactin, Peptide, Lipids and Lipoproteins: Metabolism, Regulation, and Signaling, Biology, Biochemistry, Gas Chromatography-Mass Spectrometry, Antigens, CD1, Serine, Lipopeptides, chemistry.chemical_compound, Antigen, Peptide synthesis, medicine, Humans, Receptor, Oxazoles, Molecular Biology, chemistry.chemical_classification, Lysine, Lipopeptide, Stereoisomerism, Mycobacterium tuberculosis, Cell Biology, Lipids, Butyrates, medicine.anatomical_structure, Models, Chemical, chemistry, Leukocytes, Mononuclear, Hydroxy Acids

Abstract

Mycobacterium tuberculosis survival in cells requires mycobactin siderophores. Recently, the search for lipid antigens presented by the CD1a antigen-presenting protein led to the discovery of a mycobactin-like compound, dideoxymycobactin (DDM). Here we synthesize DDMs using solution phase and solid phase peptide synthesis chemistry. Comparison of synthetic standards to natural mycobacterial mycobactins by nuclear magnetic resonance and mass spectrometry allowed identification of an unexpected alpha-methyl serine unit in natural DDM. This finding further distinguishes these pre-siderophores as foreign compounds distinct from conventional peptides, and we provide evidence that this chemical variation influences the T cell response. One synthetic DDM recapitulated natural structures and potently stimulated T cells, making it suitable for patient studies of CD1a in infectious disease. DDM analogs differing in the stereochemistry of their butyrate or oxazoline moieties were not recognized by human T cells. Therefore, we conclude that T cells show precise specificity for both arms of the peptide, which are predicted to lie at the CD1a-T cell receptor interface.

Published

2009

23. Cover Picture: Preparation and Evaluation of Potent Pentafluorosulfanyl-Substituted Anti-Tuberculosis Compounds (ChemMedChem 14/2017)

Author

Helena I. Boshoff, Patricia S. Tsang, Garrett C. Moraski, Marvin J. Miller, Ryan Bristol, and Natalie Seeger

Subjects

Pharmacology, biology, Chemistry, Organic Chemistry, Drug resistance, biology.organism_classification, Biochemistry, Virology, Mycobacterium tuberculosis, Anti tuberculosis, Drug Discovery, Molecular Medicine, Cover (algebra), General Pharmacology, Toxicology and Pharmaceutics

Published

2017

24. Advancement of Imidazo[1,2

Author

Garrett C, Moraski, Lowell D, Markley, Jeffrey, Cramer, Philip A, Hipskind, Helena, Boshoff, Mai, Bailey, Torey, Alling, Juliane, Ollinger, Tanya, Parish, and Marvin J, Miller

Abstract

A set of fourteen imidazo[1,2

Published

2013

25. A Dual Read-Out Assay to Evaluate the Potency of Compounds Active against Mycobacterium tuberculosis

Author

Stephanie Florio, Allen Casey, Juliane Ollinger, Tanya Parish, Torey Alling, Mai A. Bailey, Garrett C. Moraski, and Marvin J. Miller

Subjects

Bacterial Diseases, Drugs and Devices, Tuberculosis, medicine.drug_class, Applied Microbiology, Antibiotics, Antitubercular Agents, lcsh:Medicine, Microbial Sensitivity Tests, Microbiology, Mycobacterium tuberculosis, 03 medical and health sciences, Minimum inhibitory concentration, Diagnostic Medicine, Genes, Reporter, medicine, Potency, Structure–activity relationship, lcsh:Science, Biology, Microbial Pathogens, 030304 developmental biology, 0303 health sciences, Multidisciplinary, Chromatography, biology, 030306 microbiology, Chemistry, lcsh:R, Tropical Diseases (Non-Neglected), Reproducibility of Results, Gene Expression Regulation, Bacterial, medicine.disease, biology.organism_classification, Fluorescence, 3. Good health, Infectious Diseases, Spectrometry, Fluorescence, Medical Microbiology, Medicine, lcsh:Q, Rifampicin, medicine.drug, Research Article, Test Evaluation

Abstract

Tuberculosis is a serious global health problem caused by the bacterium Mycobacterium tuberculosis. There is an urgent need for discovery and development of new treatments, but this can only be accomplished through rapid and reproducible M. tuberculosis assays designed to identify potent inhibitors. We developed an automated 96-well assay utilizing a recombinant strain of M. tuberculosis expressing a far-red fluorescent reporter to determine the activity of novel compounds; this allowed us to measure growth by monitoring both optical density and fluorescence. We determined that optical density and fluorescence were correlated with cell number during logarithmic phase growth. Fluorescence was stably maintained without antibiotic selection over 5 days, during which time cells remained actively growing. We optimized parameters for the assay, with the final format being 5 days’ growth in 96-well plates in the presence of 2% w/v DMSO. We confirmed reproducibility using rifampicin and other antibiotics. The dual detection method allows for a reproducible calculation of the minimum inhibitory concentration (MIC), at the same time detecting artefacts such as fluorescence quenching or compound precipitation. We used our assay to confirm anti-tubercular activity and establish the structure activity relationship (SAR) around the imidazo[1,2-a]pyridine-3-carboxamides, a promising series of M. tuberculosis inhibitors.

Published

2013

26. Thiolates Chemically Induce Redox Activation of BTZ043 and Related Potent Nitro Aromatic Anti-Tuberculosis Agents

Author

Rohit Tiwari, Eliza Herrero, Garrett C. Moraski, Marvin J. Miller, Viktor Krchňák, Mariangelli Colon-Martinez, Patricia A. Miller, and Allen G. Oliver

Subjects

Oxidase test, Molecular Structure, Stereochemistry, Antitubercular Agents, Thiazines, General Chemistry, Nitroso, Biochemistry, Catalysis, Article, Multiple drug resistance, chemistry.chemical_compound, Colloid and Surface Chemistry, chemistry, Biosynthesis, Suicide inhibition, Arabinogalactan, In vivo, Reactivity (chemistry), Spiro Compounds, Sulfhydryl Compounds, Oxidation-Reduction

Abstract

The development of multidrug resistant (MDR) and extensively drug resistant (XDR) forms of tuberculosis (TB) has stimulated research efforts globally to expand the new drug pipeline. Nitro aromatic compounds, including 1, 3-Benzothiazin-4-ones (BTZs) and related agents, are a promising new class for the treatment of TB. Research has shown that the nitroso intermediates of BTZs that are generated in vivo cause suicide inhibition of decaprenylphosphoryl-β-D-ribose 2′ oxidase (DprE1), which is responsible for cell wall arabinogalactan biosynthesis. We have designed and synthesized novel anti-TB agents inspired from BTZs and other nitroaromatic compounds. Computational studies indicated that the unsubstituted aromatic carbons of BTZ043 and related nitroaromatic compounds are the most electron deficient and might be prone to nucleophilic attack. Our chemical studies on BTZ043 and the additional nitro aromatic compounds synthesized by us and the others confirmed the postulated reactivity. The results indicate that nucleophiles such as thiolates, cyanide and hydride induce non-enzymatic reduction of the nitro groups present in these compounds to the corresponding nitroso intermediates by addition at the unsubstituted electron deficient aromatic carbon present in these compounds. Furthermore we demonstrate here that these compounds are good candidates for the classical von Richter reaction. These chemical studies offer an alternate hypotheses for the mechanism of action of nitro aromatic anti-TB agents in that the cysteine thiol(ate) or a hydride source at the active site of DprE1 may trigger the reduction of the nitro groups in a manner similar to the von Richter reaction to the nitroso intermediates, to initiate the inhibition of DprE1.

Published

2013

27. Syntheses and biological studies of novel spiropiperazinyl oxazolidinone antibacterial agents using a spirocyclic diene derived acylnitroso Diels-Alder reaction

Author

Ute Möllmann, Jane A. Thanassi, Cheng Ji, Michael J. Pucci, Weimin Lin, Marvin J. Miller, Garrett C. Moraski, and Scott G. Franzblau

Subjects

Methicillin-Resistant Staphylococcus aureus, Staphylococcus aureus, Stereochemistry, medicine.drug_class, Clinical Biochemistry, Antibiotics, Drug Evaluation, Preclinical, Pharmaceutical Science, Bacillus subtilis, Microbial Sensitivity Tests, medicine.disease_cause, Gram-Positive Bacteria, Biochemistry, Enterococcus faecalis, Article, Microbiology, Cell Line, Mycobacterium, chemistry.chemical_compound, Vancomycin, Drug Discovery, Drug Resistance, Bacterial, Gram-Negative Bacteria, medicine, Humans, Molecular Biology, Oxazolidinones, Diels–Alder reaction, biology, Molecular Structure, Organic Chemistry, Nitroso, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Anti-Bacterial Agents, chemistry, Molecular Medicine, Mycobacterium vaccae, Bacteria, Enterococcus

Abstract

Several novel oxazolidinone antibiotics with a spiropiperazinyl substituent at the 4′-position of the phenyl ring were synthesized through nitroso Diels–Alder chemistry and the in vitro antibacterial activities were evaluated against various Gram-positive bacteria ( Bacillus subtilis , Staphylococcus aureus , Enterococcus faecalis ), Gram-negative bacteria ( Escherichia coli , Pseudomonas aeruginosa ) and mycobacteria ( Mycobacterium vaccae , Mycobacterium tuberculosis ). Analogs ( 8a and 12 ) were active against selected drug resistant microbes, like methicillin-resistant Staphylococcus aureus (MRSA) and vancomycin-resistant enterococci (VRE) and had no mammalian toxicity in a Hep-2 cellular assay (CC 50 >100 μM).

Published

2012

28. ChemInform Abstract: One-Step Syntheses of Nitrofuranyl Benzimidazoles that Are Active Against Multidrug-Resistant Bacteria

Author

Michael J. Pucci, Marvin J. Miller, Jane A. Thanassi, Steven D. Podos, and Garrett C. Moraski

Subjects

Multidrug resistant bacteria, biology, Chemistry, General Medicine, biology.organism_classification, Bacteria, Microbiology

Abstract

One-step syntheses of nitrofuranyl benzimidazoles that are active against multidrug-resistant bacteria

Published

2012

29. Generation and exploration of new classes of antitubercular agents: The optimization of oxazolines, oxazoles, thiazolines, thiazoles to imidazo[1,2-a]pyridines and isomeric 5,6-fused scaffolds

Author

Helena I. Boshoff, Mayland Chang, Lowell D. Markley, CH Hwang, Sang-Hyun Cho, Garrett C. Moraski, Scott G. Franzblau, and Marvin J. Miller

Subjects

Pyrimidine, Stereochemistry, Pyridines, Clinical Biochemistry, Antitubercular Agents, Pharmaceutical Science, Microbial Sensitivity Tests, Pyrazole, Biochemistry, Article, chemistry.chemical_compound, Structure-Activity Relationship, Isomerism, Drug Discovery, Pyridine, Structure–activity relationship, Isoxazole, Thiazole, Molecular Biology, Oxazoles, Oxazole, Thiazoline, Organic Chemistry, Isoxazoles, Mycobacterium tuberculosis, Combinatorial chemistry, Thiazoles, chemistry, Molecular Medicine

Abstract

Tuberculosis (TB) is a devastating disease resulting in a death every 20 seconds. Thus, new drugs are urgently needed. Herein we report ten classes of compounds—oxazoline, oxazole, thiazoline, thiazole, pyrazole, pyridine, isoxazole, imidazo[1,2-a]pyridine, imidazo[1,2-a]pyrimidine and imidazo[1,2-c]pyrimidine—which have good (micromolar) to excellent (sub-micromolar) antitubercular potency. The 5,6-fused heteroaromatic compounds were the most potent with MIC’s as low as

Published

2011

30. UTILIZTION OF THE SUZUKI COUPLING TO ENHANCE THE ANTITUBERCULOSIS ACTIVITY OF ARYL OXAZOLES

Author

Garrett C. Moraski, Scott G. Franzblau, and Marvin J. Miller

Subjects

Pharmacology, chemistry.chemical_classification, Low toxicity, Aryl halide, Aryl, Organic Chemistry, Antituberculosis agent, Coupling reaction, Article, Analytical Chemistry, chemistry.chemical_compound, Suzuki reaction, chemistry, Organic chemistry

Abstract

Potent antituberculosis aryl oxazoles can be made in an efficient three step process--formation of β-hydroxy amides with serine benzyl ester; cyclization to afford oxazolines; and then dehydration to give the corresponding oxazoles. Furthermore, incorporation of an appropriate aryl halide allows utilization of the Suzuki cross coupling reaction to access new chemical space and more elaborate analogs. The compounds prepared by this method were shown to possess improved activity against M. tuberculosis, extremely low toxicity toward VERO cells and, as a result, high therapeutic indexes.

Published

2011

31. One-step syntheses of nitrofuranyl benzimidazoles that are active against multidrug-resistant bacteria

Author

Michael J. Pucci, Steven D. Podos, Marvin J. Miller, Jane A. Thanassi, and Garrett C. Moraski

Subjects

Benzimidazole, Veterinary medicine, medicine.drug_class, VRE, Antibiotics, MRSA, nitrofuran, 01 natural sciences, Article, benzimidazole, Microbiology, 03 medical and health sciences, chemistry.chemical_compound, antibiotic, Drug Discovery, Medicine, Nitrofuran, Pharmacology, 0303 health sciences, biology, 010405 organic chemistry, 030306 microbiology, business.industry, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, 3. Good health, 0104 chemical sciences, Multidrug resistant bacteria, chemistry, business, Bacteria

Abstract

Nitrofuranyl benzimidazoles can be made in one synthetic step from commercially available starting materials. The compounds displayed unexpected antibacterial activity against methicillin-resistant Staphylococcus aureus (MSRA) and vancomycin-resistant Enterococcus faecium (VRE) with MICs as low as ~1 µg/ml.

Published

2011

32. Advent of Imidazo[1,2-a]pyridine-3-carboxamides with Potent Multi- and Extended Drug Resistant Antituberculosis Activity

Author

Sang-Hyun Cho, Lowell D. Markley, Marvin J. Miller, Scott G. Franzblau, Garrett C. Moraski, Helena I. Boshoff, and Philip Arthur Hipskind

Subjects

business.industry, Drug resistant tuberculosis, Organic Chemistry, Drug resistance, Pharmacology, Biochemistry, In vitro, chemistry.chemical_compound, chemistry, In vivo, Drug Discovery, Pyridine, Medicine, Potency, business, ADME

Abstract

A set of nine 2,7-dimethylimidazo[1,2-a]pyridine-3-carboxamides and one 2,6-dimethylimidazo[1,2-a]pyrimidine-3-carboxamide were synthesized. The compounds were evaluated for their in vitro anti-tuberculosis activity versus replicating, non-replicating, multi- and extensive drug resistant Mtb strains. The MIC(90) values of seven of these agents were ≤ 1 μM against the various tuberculosis strains tested. A representative compound of this class (1) was screened against seven non-tubercular strains as well as other non-mycobacteria organisms and demonstrated remarkable microbe selectivity. A transcriptional profiling experiment of Mtb treated with compound 1 was performed to give a preliminary indication of the mode of action. Lastly, the in vivo ADME properties of compounds 1, 3, 4, and 6 were assessed. The 2,7-dimethylimidazo[1,2-a]pyridine-3-carboxamides are a drug-like and synthetically accessible class of anti-TB agents that have excellent selective potency against multi- and extensive drug resistant TB and encouraging pharmacokinetics.

Published

2011

33. ChemInform Abstract: Utilization of the Suzuki Coupling to Enhance the Antituberculosis Activity of Aryloxazoles

Author

Scott G. Franzblau, Marvin J. Miller, and Garrett C. Moraski

Subjects

chemistry.chemical_compound, chemistry, Suzuki reaction, Aryl, General Medicine, Combinatorial chemistry

Abstract

A three-step process enables access to aryl oxazoles via formation of β-hydroxy amides (III), cyclization to oxazolines (IV), and dehydration to provide oxazoles (V).

Published

2010

34. N-((1-benzyl-1H-1,2,3-triazol-4-yl)methyl)arylamide as a new scaffold that provides rapid access to antimicrotubule agents: synthesis and evaluation of antiproliferative activity against select cancer cell lines

Author

Rebecca J. Peterson, Rahul Palchaudhuri, Patricia A. Miller, Jonathan A. Stefely, Paul J. Hergenrother, Garrett C. Moraski, and Marvin J. Miller

Subjects

G2 Phase, Stereochemistry, Microtubules, Article, Flow cytometry, HeLa, chemistry.chemical_compound, Structure-Activity Relationship, Tubulin, Cell Line, Tumor, Drug Discovery, medicine, Structure–activity relationship, Humans, Oxazoles, Acrylamides, medicine.diagnostic_test, biology, Tubulin Modulators, Triazoles, biology.organism_classification, Paclitaxel, chemistry, Biochemistry, Cell culture, Cancer cell, biology.protein, Molecular Medicine, Drug Screening Assays, Antitumor, Cell Division

Abstract

A series of N-((1-benzyl-1H-1,2,3-triazol-4-yl)methyl)arylamides was synthesized by copper-catalyzed azide-alkyne cycloaddition (CuAAC) and afforded inhibitors of cancer cell growth. For example, compound 13e had an IC(50) of 46 nM against MCF-7 human breast tumor cells. Structure-activity relationship (SAR) studies demonstrated that (i) meta-phenoxy substitution of the N-1-benzyl group is important for antiproliferative activity and (ii) a variety of heterocyclic substitutions for the aryl group of the arylamide are tolerated. In silico COMPARE analysis of antiproliferative activity against the NCI-60 human tumor cell line panel revealed a correlation to clinically useful antimicrotubule agents such as paclitaxel and vincristine. This in silico correlation was supported by (i) in vitro inhibition of tubulin polymerization, (ii) G(2)/M-phase arrest in HeLa cells as assessed by flow cytometry, and (iii) perturbation of normal microtubule activity in HeLa cells as observed by confocal microscopy. The results demonstrate that N-((1-benzyl-1H-1,2,3-triazol-4-yl)methyl)arylamide is a readily accessible small molecule scaffold for compounds that inhibit tubulin polymerization and tumor cell growth.

Published

2010

35. Structure-activity relationship of new anti-tuberculosis agents derived from oxazoline and oxazole benzyl esters

Author

Adriel Villegas-Estrada, Garrett C. Moraski, Marvin J. Miller, Scott G. Franzblau, Ute Möllmann, and Maylland Chang

Subjects

Stereochemistry, Antitubercular Agents, Drug Evaluation, Preclinical, Molecular Conformation, Mycobactin, Oxazoline, Chemical synthesis, Article, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Drug Discovery, Structure–activity relationship, Animals, Tuberculosis, Oxazoles, Oxazole, ADME, Antibacterial agent, Pharmacology, Mice, Inbred BALB C, Chemistry, Organic Chemistry, Esters, Stereoisomerism, General Medicine, Mycobacterium tuberculosis, Small molecule, Disease Models, Animal

Abstract

During the syntheses and studies of natural iron chelators (mycobactins), we serendipitously discovered that a simple, small molecule, oxazoline-containing intermediate 3 displayed surprising anti-tuberculosis activity (MIC of 7.7 μM, average). Herein we report elaboration of SAR around this hit as well as the syntheses and evaluation of a hundred oxazoline- and oxazole-containing compounds derived from an efficient three step process: 1) formation of β-hydroxy amides with serine or threonine; 2) cyclization to afford oxazolines; and 3) dehydration to give the corresponding oxazoles. A number of compounds prepared by this method were shown to possess impressive activity against Mycobacterium tuberculosis, extremely low toxicity and therefore high therapeutic indexes, as well as activity against even the more recalcitrant non-replicating form of M. tuberculosis. The uniqueness of their structures and their simplicity should allow them to be further optimized to meet ADME (absorption, distribution, metabolism, excretion) requirements. The syntheses of eight of the most potent in vitro compounds were scaled up and the compounds were tested in an in vivo mouse infection model to evaluate their efficacy before engaging upon more elaborate compound design and optimization.

Published

2009

36. Highly Efficient Microwave-Assisted Synthesis of 2-Arylimidazo[1,2-a]Pyridine-3-Carbaldehydes in PEG-400.

Author

Yeslam Saeed Atif, Hani, Mohsin, Mohammad, and Durrani, Ayesha N.

Subjects

ORGANIC solvents, MICROWAVES, IMIDAZOPYRIDINES, IRRADIATION

Abstract

We have designed a simple and efficient method for the synthesis of 2-Arylimidazo[1,2-a]pyridine-3-carbaldehyde from imidazo[1,2-a]pyridines with a mixture of DMF and POCl3 in presence of PEG-400 as a green reaction medium under microwave irradiation at 400 watt, and 90 0C. The main advantages of this protocol compared to other previously developed methods, were its mild reaction condition, high yield percentage, short reaction time, clean reaction profile, and avoidance of toxic catalysts, hazardous organic solvents, and waste production. [ABSTRACT FROM AUTHOR]

Published

2023

37. Syntheses and Structure–Activity Relationships of N -Phenethyl-Quinazolin-4-yl-Amines as Potent Inhibitors of Cytochrome bd Oxidase in Mycobacterium tuberculosis.

Author

Hopfner, Sarah M., Lee, Bei Shi, Kalia, Nitin P., Miller, Marvin J., Pethe, Kevin, and Moraski, Garrett C.

Subjects

STRUCTURE-activity relationships, MYCOBACTERIUM tuberculosis, MYCOBACTERIUM bovis, TUBERCULOSIS, CYTOCHROME c

Abstract

The development of cytochrome bd oxidase (cyt-bd) inhibitors are needed for comprehensive termination of energy production in Mycobacterium tuberculosis (Mtb) to treat tuberculosis infections. Herein, we report on the structure-activity-relationships (SAR) of 22 new N-phenethyl-quinazolin-4-yl-amines that target cyt-bd. Our focused set of compounds was synthesized and screened against three mycobacterial strains: Mycobacterium bovis BCG, Mycobacterium tuberculosis H37Rv and the clinical isolate Mycobacterium tuberculosis N0145 with and without the cytochrome bcc:aa3 inhibitor Q203 in an ATP depletion assay. Two compounds, 12a and 19a, were more active against all three strains than the naturally derived cyt-bd inhibitor aurachin D. [ABSTRACT FROM AUTHOR]

Published

2021

38. Dual inhibition of the terminal oxidases eradicates antibiotic‐tolerant Mycobacterium tuberculosis.

Author

Lee, Bei Shi, Hards, Kiel, Engelhart, Curtis A, Hasenoehrl, Erik J, Kalia, Nitin P, Mackenzie, Jared S, Sviriaeva, Ekaterina, Chong, Shi Min Sherilyn, Manimekalai, Malathy Sony S, Koh, Vanessa H, Chan, John, Xu, Jiayong, Alonso, Sylvie, Miller, Marvin J, Steyn, Adrie J C, Grüber, Gerhard, Schnappinger, Dirk, Berney, Michael, Cook, Gregory M, and Moraski, Garrett C

Abstract

The approval of bedaquiline has placed energy metabolism in the limelight as an attractive target space for tuberculosis antibiotic development. While bedaquiline inhibits the mycobacterial F1F0 ATP synthase, small molecules targeting other components of the oxidative phosphorylation pathway have been identified. Of particular interest is Telacebec (Q203), a phase 2 drug candidate inhibitor of the cytochrome bcc:aa3 terminal oxidase. A functional redundancy between the cytochrome bcc:aa3 and the cytochrome bd oxidase protects M. tuberculosis from Q203‐induced death, highlighting the attractiveness of the bd‐type terminal oxidase for drug development. Here, we employed a facile whole‐cell screen approach to identify the cytochrome bd inhibitor ND‐011992. Although ND‐011992 is ineffective on its own, it inhibits respiration and ATP homeostasis in combination with Q203. The drug combination was bactericidal against replicating and antibiotic‐tolerant, non‐replicating mycobacteria, and increased efficacy relative to that of a single drug in a mouse model. These findings suggest that a cytochrome bd oxidase inhibitor will add value to a drug combination targeting oxidative phosphorylation for tuberculosis treatment. Synopsis: The functional redundancy of two terminal oxidases in mycobacteria limits the efficacy of phase 2 clinical candidate Telacebec (Q203). In this study we identified a cytochrome bd oxidase inhibitor ND‐011992 that together with Q203 forms a bactericidal drug combination against Mycobacterium tuberculosis. ND‐011992 was identified and validated as an inhibitor of the Cytochrome bd oxidase.ND‐011992 and Q203 jointly enhanced inhibition of oxygen respiration, intracellular ATP depletion, and bactericidal activity.The drug combination was active against M. tuberculosis clinical isolates of various lineages as well as against MDR‐ and XDR‐TB isolates.The addition of ND‐011992 to Q203 treatment did not significantly alter the frequency of resistance to treatment, suggesting there is limited added risk of rapid emergence of escape mutants.The ND‐011992‐Q203 combination showed enhanced killing effect in the animal study compared to that of single drugs, demonstrating translatability in an in vivo model. [ABSTRACT FROM AUTHOR]

Published

2021

39. Intracellular and in vivo evaluation of imidazo[2,1-b]thiazole-5-carboxamide anti-tuberculosis compounds.

Author

Moraski, Garrett C., Deboosère, Nathalie, Marshall, Kate L., Weaver, Heath A., Vandeputte, Alexandre, Hastings, Courtney, Woolhiser, Lisa, Lenaerts, Anne J., Brodin, Priscille, and Miller, Marvin J.

Subjects

COMBINATION drug therapy, DRUG development, IMIDAZOPYRIDINES, ELECTRON transport, PROTEIN binding, ISOINDOLE, BIOCHEMICAL mechanism of action

Abstract

The imidazo[2,1-b]thiazole-5-carboxamides (ITAs) are a promising class of anti-tuberculosis agents shown to have potent activity in vitro and to target QcrB, a key component of the mycobacterial cytochrome bcc-aa3 super complex critical for the electron transport chain. Herein we report the intracellular macrophage potency of nine diverse ITA analogs with MIC values ranging from 0.0625–2.5 μM and mono-drug resistant potency ranging from 0.0017 to 7 μM. The in vitro ADME properties (protein binding, CaCo-2, human microsomal stability and CYP450 inhibition) were determined for an outstanding compound of the series, ND-11543. ND-11543 was tolerable at >500 mg/kg in mice and at a dose of 200 mg/kg displayed good drug exposure in mice with an AUC(0-24h) >11,700 ng·hr/mL and a >24 hr half-life. Consistent with the phenotype observed with other QcrB inhibitors, compound ND-11543 showed efficacy in a chronic murine TB infection model when dosed at 200 mg/kg for 4 weeks. The efficacy was not dependent upon exposure, as pre-treatment with a known CYP450-inhibitor did not substantially improve efficacy. The ITAs are an interesting scaffold for the development of new anti-TB drugs especially in combination therapy based on their favorable properties and novel mechanism of action. [ABSTRACT FROM AUTHOR]

Published

2020

40. Plasticity of the Mycobacterium tuberculosis respiratory chain and its impact on tuberculosis drug development.

Author

Beites, Tiago, O'Brien, Kathryn, Tiwari, Divya, Engelhart, Curtis A., Walters, Shaun, Andrews, Jenna, Yang, Hee-Jeong, Sutphen, Michelle L., Weiner, Danielle M., Dayao, Emmanuel K., Zimmerman, Matthew, Prideaux, Brendan, Desai, Prashant V., Masquelin, Thierry, Via, Laura E., Dartois, Véronique, Boshoff, Helena I., Barry III, Clifton E., Ehrt, Sabine, and Schnappinger, Dirk

Subjects

PHENOTYPIC plasticity, MYCOBACTERIUM tuberculosis, CYTOCHROMES, DEHYDROGENASES, DRUG development

Abstract

The viability of Mycobacterium tuberculosis (Mtb) depends on energy generated by its respiratory chain. Cytochrome bc1-aa3 oxidase and type-2 NADH dehydrogenase (NDH-2) are respiratory chain components predicted to be essential, and are currently targeted for drug development. Here we demonstrate that an Mtb cytochrome bc1-aa3 oxidase deletion mutant is viable and only partially attenuated in mice. Moreover, treatment of Mtb-infected marmosets with a cytochrome bc1-aa3 oxidase inhibitor controls disease progression and reduces lesion-associated inflammation, but most lesions become cavitary. Deletion of both NDH-2 encoding genes (Δndh-2 mutant) reveals that the essentiality of NDH-2 as shown in standard growth media is due to the presence of fatty acids. The Δndh-2 mutant is only mildly attenuated in mice and not differently susceptible to clofazimine, a drug in clinical use proposed to engage NDH-2. These results demonstrate the intrinsic plasticity of Mtb's respiratory chain, and highlight the challenges associated with targeting the pathogen's respiratory enzymes for tuberculosis drug development. New tuberculosis therapies, targeting respiratory chain components of Mycobacterium tuberculosis, are under development. Here the authors show that, contrary to common belief, some of these components are not essential for pathogen viability and/or virulence in animal models of infection. [ABSTRACT FROM AUTHOR]

Published

2019

41. Cover Picture: Preparation and Evaluation of Potent Pentafluorosulfanyl-Substituted Anti-Tuberculosis Compounds (ChemMedChem 14/2017).

Author

Moraski, Garrett C., Bristol, Ryan, Seeger, Natalie, Boshoff, Helena I., Tsang, Patricia Siu‐Yee, and Miller, Marvin J.

Published

2017

42. Preparation and Evaluation of Potent Pentafluorosulfanyl-Substituted Anti-Tuberculosis Compounds.

Author

Moraski, Garrett C., Bristol, Ryan, Seeger, Natalie, Boshoff, Helena I., Tsang, Patricia Siu‐Yee, and Miller, Marvin J.

Published

2017

43. Bactericidal Activity of an Imidazo[1, 2-a]pyridine Using a Mouse M. tuberculosis Infection Model.

Author

Cheng, Yong, Moraski, Garrett C., Cramer, Jeffrey, Miller, Marvin J., and Schorey, Jeffrey S.

Subjects

IMIDAZOPYRIDINES, BACTERICIDES, MYCOBACTERIUM tuberculosis, LABORATORY mice, DRUG resistance, ANTITUBERCULAR agents

Abstract

Tuberculosis remains a global threat due in part to the long treatment regimen and the increased prevalence of drug resistant M. tuberculosis strains. Therefore, new drug regimens are urgently required to combat this deadly disease. We previously synthesized and evaluated a series of new anti-tuberculosis compounds which belong to the family of imidazo[1,2-a]pyridines. This family of compounds showed low nM MIC (minimal inhibitory concentration) values against M. tuberculosis in vitro. In this study, a derivative of imidazo[1,2-a]pyridines, (N-(4-(4-chlorophenoxy)benzyl)-2,7-dimethylimidazo[1,2-a]pyridine-3-carboxamide) (ND-09759), was selected as a promising lead compound to determine its protective efficacy using a mouse infection model. Pharmacokinetic analysis of ND-09759 determined that at a dosage of 30 mg/kg mouse body weight (PO) gave a maximum serum drug concentration (Cmax) of 2.9 µg/ml and a half-life of 20.1 h. M. tuberculosis burden in the lungs and spleens was significantly decreased in mice treated once daily 6 days per week for 4-weeks with ND-09759 compared to untreated mice and this antibiotic activity was equivalent to isoniazid (INH) and rifampicin (RMP), two first-line anti-TB drugs. We observed slightly higher efficacy when using a combination of ND-09759 with either INH or RMP. Finally, the histopathological analysis revealed that infected mice treated with ND-09759 had significantly reduced inflammation relative to untreated mice. In conclusion, our findings indicate ND-09759 might be a potent candidate for the treatment of active TB in combination with current standard anti-TB drugs. [ABSTRACT FROM AUTHOR]

Published

2014

44. A Dual Read-Out Assay to Evaluate the Potency of Compounds Active against Mycobacterium tuberculosis.

Author

Ollinger, Juliane, Bailey, Mai Ann, Moraski, Garrett C., Casey, Allen, Florio, Stephanie, Alling, Torey, Miller, Marvin J., and Parish, Tanya

Subjects

MYCOBACTERIUM tuberculosis, MEDICAL microbiology, PATHOGENIC microorganisms, BACTERIAL diseases, COMMUNICABLE diseases, ANTITUBERCULAR agents, FLUORESCENCE, OPACITY (Optics)

Abstract

Tuberculosis is a serious global health problem caused by the bacterium Mycobacterium tuberculosis. There is an urgent need for discovery and development of new treatments, but this can only be accomplished through rapid and reproducible M. tuberculosis assays designed to identify potent inhibitors. We developed an automated 96-well assay utilizing a recombinant strain of M. tuberculosis expressing a far-red fluorescent reporter to determine the activity of novel compounds; this allowed us to measure growth by monitoring both optical density and fluorescence. We determined that optical density and fluorescence were correlated with cell number during logarithmic phase growth. Fluorescence was stably maintained without antibiotic selection over 5 days, during which time cells remained actively growing. We optimized parameters for the assay, with the final format being 5 days’ growth in 96-well plates in the presence of 2% w/v DMSO. We confirmed reproducibility using rifampicin and other antibiotics. The dual detection method allows for a reproducible calculation of the minimum inhibitory concentration (MIC), at the same time detecting artefacts such as fluorescence quenching or compound precipitation. We used our assay to confirm anti-tubercular activity and establish the structure activity relationship (SAR) around the imidazo[1,2-a]pyridine-3-carboxamides, a promising series of M. tuberculosis inhibitors. [ABSTRACT FROM AUTHOR]

Published

2013

45. Carbon metabolism modulates the efficacy of drugs targeting the cytochrome bc1:aa3 in Mycobacterium tuberculosis.

Author

Kalia, Nitin P., Shi Lee, Bei, Ab Rahman, Nurlilah B., Moraski, Garrett C., Miller, Marvin J., and Pethe, Kevin

Abstract

The influence of carbon metabolism on oxidative phosphorylation is poorly understood in mycobacteria. M. tuberculosis expresses two respiratory terminal oxidases, the cytochrome bc1:aa3 and the cytochrome bd oxidase, which are jointly required for oxidative phosphorylation and mycobacterial viability. The essentiality of the cytochrome bc1:aa3 for optimum growth is illustrated by its vulnerability to chemical inhibition by the clinical drug candidate Q203 and several other chemical series. The cytochrome bd oxidase is not strictly essential for growth but is required to maintain bioenergetics when the function of the cytochrome bc1:aa3 is compromised. In this study, we observed that the potency of drugs targeting the cytochrome bc1:aa3 is influenced by carbon metabolism. The efficacy of Q203 and related derivatives was alleviated by glycerol supplementation. The negative effect of glycerol supplementation on Q203 potency correlated with an upregulation of the cytochrome bd oxidase-encoding cydABDC operon. Upon deletion of cydAB, the detrimental effect of glycerol on the potency of Q203 was abrogated. The same phenomenon was also observed in recent clinical isolates, but to a lesser extent compared to the laboratory-adapted strain H37Rv. This study reinforces the importance of optimizing in vitro culture conditions for drug evaluation in mycobacteria, a factor which appeared to be particularly essential for drugs targeting the cytochrome bc1:aa3 terminal oxidase. [ABSTRACT FROM AUTHOR]

Published

2019

46. Targeting the Mycobacterium ulcerans cytochrome bc1:aa3 for the treatment of Buruli ulcer.

Author

Scherr, Nicole, Bieri, Raphael, Thomas, Sangeeta S., Chauffour, Aurélie, Kalia, Nitin Pal, Schneide, Paul, Ruf, Marie-Thérèse, Lamelas, Araceli, Manimekalai, Malathy S. S., Grüber, Gerhard, Ishii, Norihisa, Suzuki, Koichi, Tanner, Marcel, Moraski, Garrett C., Miller, Marvin J., Witschel, Matthias, Jarlier, Vincent, Pluschke, Gerd, and Pethe, Kevin

Abstract

Mycobacterium ulcerans is the causative agent of Buruli ulcer, a neglected tropical skin disease that is most commonly found in children from West and Central Africa. Despite the severity of the infection, therapeutic options are limited to antibiotics with severe side effects. Here, we show that M. ulcerans is susceptible to the anti-tubercular drug Q203 and related compounds targeting the respiratory cytochrome bc1:aa3. While the cytochrome bc1:aa3 is the primary terminal oxidase in Mycobacterium tuberculosis, the presence of an alternate bd-type terminal oxidase limits the bactericidal and sterilizing potency of Q203 against this bacterium. M. ulcerans strains found in Buruli ulcer patients from Africa and Australia lost all alternate terminal electron acceptors and rely exclusively on the cytochrome bc1:aa3 to respire. As a result, Q203 is bactericidal at low dose against M. ulcerans replicating in vitro and in mice, making the drug a promising candidate for Buruli ulcer treatment. Mycobacterium ulcerans is the causative agent of Buruli ulcer (BU). Existing anti-tubercular drugs have been used to treat the condition with varying success. Here, the authors show that a clinical-stage drug candidate for tuberculosis, Q203, is effective at killing M. ulcerans and is a promising therapeutic candidate for BU. [ABSTRACT FROM AUTHOR]

Published

2018

47. Advances in Medicine and Biology. Volume 151

Author

Leon V. Berhardt and Leon V. Berhardt

Abstract

Advances in Medicine and Biology. Volume 151 begins with a focus on one of the rapidly growing mycobacteria groups, Mycobacterium smegmatis, used to understand the pathogenesis of Mycobacterium tuberculosis because of the disadvantages in the direct study of tubercle bacilli. The authors propose that a perspective group in the current research and development of novel chemotherapeutic agents with a broad spectrum of activities may be functionalized phenolic derivatives and their metal complexes. The authors also discuss Aeromonadaceae, Gram-negative, rod-shaped bacteria which are ubiquitous in aquatic environments, but they have been also isolated from different types of both fresh and processed foods. Aeromonas species are considered opportunistic pathogens of both aquatic and terrestrial animals. Following this, the role of mannans within Candida biofilms is examined, and the role of Candida biofilms in fungal structure, pathogenesis, and resistance is also addressed. To optimize the application of ß-mannanase in practical animal nutrition, factors affecting its effectiveness have to be carefully considered. As such, the authors explore the impact of these factors on efficacy of ß-mannanase in the penultimate chapter. The concluding chapter focuses on postoperative nausea and vomiting, common and distressing side effects following surgery and anesthesia. Despite modern antiemetic agents, short-acting anesthetics and minimally invasive surgery, postoperative nausea and vomiting still affects around 30% of surgical patients, with certain high-risk patients experiencing postoperative nausea and vomiting up to 80%.

Published

2019

48. Study Results from University of Notre Dame in the Area of Tuberculosis Reported (Syntheses and Studies of Deuterated Imdiazo[1,2-a]Pyridine-3-carboxamides With Potent Anti-tuberculosis Activity and Improved Metabolic Properties)

Subjects

United States. National Institutes of Health, Pyridine -- Research, Tuberculosis -- Research, Health, University of Notre Dame

Abstract

2022 NOV 29 (NewsRx) -- By a News Reporter-Staff News Editor at TB & Outbreaks Week -- Investigators publish new report on Mycobacterium Infections - Tuberculosis. According to news reporting [...]

Published

2022

49. Studies from Montana State University Further Understanding of Mycobacterium tuberculosis (Syntheses and Structure-activity Relationships of N-phenethyl-quinazolin-4-yl-amines As Potent Inhibitors of Cytochrome Bd Oxidase In Mycobacterium ...)

Subjects

BCG vaccines -- Research, BCG -- Research, Tuberculosis -- Research, Oxidases -- Research, Amines -- Research, Health, Montana State University

Abstract

2021 NOV 23 (NewsRx) -- By a News Reporter-Staff News Editor at TB & Outbreaks Week -- Investigators publish new report on Gram-Positive Bacteria - Mycobacterium tuberculosis. According to news [...]

Published

2021

50. Recent Studies from Montana State University Add New Data to Mycobacterium tuberculosis (Structure Guided Generation of Thieno[3,2-d] Pyrimidin-4-amine Mycobacterium Tuberculosis Bd Oxidase Inhibitors)

Subjects

Medical research -- Physiological aspects, Medicine, Experimental -- Physiological aspects, BCG vaccines -- Research, BCG -- Research, Tuberculosis -- Research, Oxidases -- Physiological aspects -- Research, Amines -- Research -- Physiological aspects, Health, Montana State University

Abstract

2021 MAR 23 (NewsRx) -- By a News Reporter-Staff News Editor at TB & Outbreaks Week -- Researchers detail new data in Gram-Positive Bacteria - Mycobacterium tuberculosis. According to news [...]

Published

2021