Your search keyword '"Anna M. Upton"' showing total 29 results

1. Lysyl-tRNA synthetase, a target for urgently needed M. tuberculosis drugs

Author

Simon R. Green, Susan H. Davis, Sebastian Damerow, Curtis A. Engelhart, Michael Mathieson, Beatriz Baragaña, David A. Robinson, Jevgenia Tamjar, Alice Dawson, Fabio K. Tamaki, Kirsteen I. Buchanan, John Post, Karen Dowers, Sharon M. Shepherd, Chimed Jansen, Fabio Zuccotto, Ian H. Gilbert, Ola Epemolu, Jennifer Riley, Laste Stojanovski, Maria Osuna-Cabello, Esther Pérez-Herrán, María José Rebollo, Laura Guijarro López, Patricia Casado Castro, Isabel Camino, Heather C. Kim, James M. Bean, Navid Nahiyaan, Kyu Y. Rhee, Qinglan Wang, Vee Y. Tan, Helena I. M. Boshoff, Paul J. Converse, Si-Yang Li, Yong S. Chang, Nader Fotouhi, Anna M. Upton, Eric L. Nuermberger, Dirk Schnappinger, Kevin D. Read, Lourdes Encinas, Robert H. Bates, Paul G. Wyatt, and Laura A. T. Cleghorn

Subjects

Science

Abstract

Tuberculosis is a major cause of mortality, and the rise of drug-resistant strains of Mycobacterium tuberculosis requires the urgent development of safe and effective treatments. In this work, the authors develop a compound against lysyl-tRNA synthetase, demonstrating on-target mechanism of action and efficacy in vivo.

Published

2022

2. The Novel Oxazolidinone TBI-223 Is Effective in Three Preclinical Mouse Models of Methicillin-Resistant Staphylococcus aureus Infection

Author

Oren Gordon, Dustin A. Dikeman, Roger V. Ortines, Yu Wang, Christine Youn, Mohammed Mumtaz, Nicholas Orlando, Jeffrey Zhang, Aman M. Patel, Ethan Gough, Amit Kaushik, Eric L. Nuermberger, Anna M. Upton, Nader Fotouhi, Lloyd S. Miller, and Nathan K. Archer

Subjects

Staphylococcus aureus, antibiotic resistance, oxazolidinones, Microbiology, QR1-502

Abstract

ABSTRACT Staphylococcus aureus is an important cause of various infections in humans, including bacteremia, skin and soft tissue infections, and infections associated with implanted medical devices. The emergence of hospital- and community-acquired methicillin-resistant Staphylococcus aureus (MRSA) underscores the urgent and unmet need to develop novel, safe, and effective antibiotics against these multidrug-resistant clinical isolates. Oxazolidinone antibiotics such as linezolid have excellent oral bioavailability and provide coverage against MRSA infections. However, their widespread and long-term use is often limited by adverse effects, especially myelosuppression. TBI-223 is a novel oxazolidinone with potentially reduced myelosuppression, compared to linezolid, but its efficacy against MRSA infections is unknown. Therefore, the preclinical efficacy of TBI-223 (80 and 160 mg/kg twice daily) was compared with that of linezolid (40 and 80 mg/kg twice daily) and sham treatment in mouse models of MRSA bacteremia, skin wound infection, and orthopedic-implant-associated infection. The dosage was selected based on mouse pharmacokinetic analysis of both linezolid and TBI-223, as well as measurement of the MICs. In all three models, TBI-223 and linezolid had comparable dose-dependent efficacies in reducing bacterial burden and disease severity, compared with sham-treated control mice. Taken together, these findings indicate that TBI-223 represents a novel oxazolidinone antibiotic that may provide an additional option against MRSA infections. Future studies in larger animal models and clinical trials are warranted to translate these findings to humans. IMPORTANCE Staphylococcus aureus is the predominant cause of bloodstream, skin, and bone infections in humans. Resistance to commonly used antibiotics is a growing concern, making it more difficult to treat staphylococcal infections. Use of the oxazolidinone antibiotic linezolid against resistant strains is hindered by high rates of adverse reactions during prolonged therapy. Here, a new oxazolidinone named TBI-223 was tested against S. aureus in three mouse models of infection, i.e., bloodstream infection, skin infection, and bone infection. We found that TBI-223 was as effective as linezolid in these three models. Previous data suggest that TBI-223 has a better safety profile than linezolid. Taken together, these findings indicate that this new agent may provide an additional option against MRSA infections. Future studies in larger animal models and clinical trials are warranted to translate these findings to humans.

Published

2022

3. Synergistic Activity of Nitroimidazole-Oxazolidinone Conjugates against Anaerobic Bacteria

Author

Zhijun Zhuang, Dawei Wan, Jun Ding, Shijie He, Qian Zhang, Xiaomei Wang, Ying Yuan, Yu Lu, Charles Z. Ding, Anthony Simon Lynch, Anna M. Upton, Christopher B. Cooper, William A. Denny, and Zhenkun Ma

Subjects

drug conjugates, anaerobic bacterium, synergy, nitroimidazole and oxazolidinone, Organic chemistry, QD241-441

Abstract

The introductions of the bicyclic 4-nitroimidazole and the oxazolidinone classes of antimicrobial agents represented the most significant advancements in the infectious disease area during the past two decades. Pretomanid, a bicyclic 4-nitroimidazole, and linezolid, an oxazolidinone, are also part of a combination regimen approved recently by the US Food and Drug Administration for the treatment of pulmonary, extensively drug resistant (XDR), treatment-intolerant or nonresponsive multidrug-resistant (MDR) Mycobacterium tuberculosis (TB). To identify new antimicrobial agents with reduced propensity for the development of resistance, a series of dual-acting nitroimidazole-oxazolidinone conjugates were designed, synthesized and evaluated for their antimicrobial activity. Compounds in this conjugate series have shown synergistic activity against a panel of anaerobic bacteria, including those responsible for serious bacterial infections.

Published

2020

4. Synthetic Studies to Help Elucidate the Metabolism of the Preclinical Candidate TBAJ-876—A Less Toxic and More Potent Analogue of Bedaquiline

Author

Peter J. Choi, Daniel Conole, Hamish S. Sutherland, Adrian Blaser, Amy S.T. Tong, Christopher B. Cooper, Anna M. Upton, Brian D. Palmer, and William A. Denny

Subjects

bedaquiline, tmc207, sirturo, bedaquiline analogues, tbaj-876, mycobacterium tuberculosis, tuberculosis, drug development, Organic chemistry, QD241-441

Abstract

Bedaquiline is a novel drug approved in 2012 by the FDA for treatment of drug-resistant tuberculosis (TB). Although it shows high efficacy towards drug-resistant forms of TB, its use has been limited by the potential for significant side effects. In particular, bedaquiline is a very lipophilic compound with an associated long terminal half-life and shows potent inhibition of the cardiac potassium hERG channel, resulting in QTc interval prolongation in humans that may result in cardiac arrhythmia. To address these issues, we carried out a drug discovery programme to develop an improved second generation analogue of bedaquiline. From this medicinal chemistry program, a candidate (TBAJ-876) has been selected to undergo further preclinical evaluation. During this evaluation, three major metabolites arising from TBAJ-876 were observed in several preclinical animal models. We report here our synthetic efforts to unequivocally structurally characterize these three metabolites through their independent directed synthesis.

Published

2020

5. 'Upcycling' known molecules and targets for drug-resistant TB

Author

Christine Roubert, Evelyne Fontaine, and Anna M Upton

Subjects

drug resistance, target, antibiotics, phenotypic screening, golden age of antibiotics, Microbiology, QR1-502

Abstract

Despite reinvigorated efforts in Tuberculosis (TB) drug discovery over the past 20 years, relatively few new drugs and candidates have emerged with clear utility against drug resistant TB. Over the same period, significant technological advances and learnings around target value have taken place. This has offered opportunities to re-assess the potential for optimization of previously discovered chemical matter against Mycobacterium tuberculosis (M.tb) and for reconsideration of clinically validated targets encumbered by drug resistance. A re-assessment of discarded compounds and programs from the “golden age of antibiotics” has yielded new scaffolds and targets against TB and uncovered classes, for example beta-lactams, with previously unappreciated utility for TB. Leveraging validated classes and targets has also met with success: booster technologies and efforts to thwart efflux have improved the potential of ethionamide and spectinomycin classes. Multiple programs to rescue high value targets while avoiding cross-resistance are making progress. These attempts to make the most of known classes, drugs and targets complement efforts to discover new chemical matter against novel targets, enhancing the chances of success of discovering effective novel regimens against drug-resistant TB.

Published

2022

6. Identification of 2-Aryl-Quinolone Inhibitors of Cytochrome bd and Chemical Validation of Combination Strategies for Respiratory Inhibitors against Mycobacterium tuberculosis

Author

Laura N. Jeffreys, Alison Ardrey, Taghreed A. Hafiz, Lauri-Anne Dyer, Ashley J. Warman, Nada Mosallam, Gemma L. Nixon, Nicholas E. Fisher, W. David Hong, Suet C. Leung, Ghaith Aljayyoussi, Jaclyn Bibby, Deepak V. Almeida, Paul J. Converse, Nader Fotouhi, Neil G. Berry, Eric L. Nuermberger, Anna M. Upton, Paul M. O’Neill, Stephen A. Ward, and Giancarlo A. Biagini

Subjects

Infectious Diseases

Published

2023

7. Delamanid or pretomanid?

Author

Saskia E. Mudde, Anna M. Upton, Anne Lenaerts, Hannelore I. Bax, Jurriaan E. M. De Steenwinkel, Medical Microbiology & Infectious Diseases, and Internal Medicine

Subjects

Pharmacology, Microbiology (medical), Infectious Diseases, SDG 3 - Good Health and Well-being, Nitroimidazoles, Tuberculosis, Multidrug-Resistant, Antitubercular Agents, Humans, Pharmacology (medical), Mycobacterium tuberculosis, Diarylquinolines, Oxazoles

Abstract

Given the low treatment success rates of drug-resistant tuberculosis (TB), novel TB drugs are urgently needed. The landscape of TB treatment has changed considerably over the last decade with the approval of three new compounds: bedaquiline, delamanid and pretomanid. Of these, delamanid and pretomanid belong to the same class of drugs, the nitroimidazoles. In order to close the knowledge gap on how delamanid and pretomanid compare with each other, we summarize the main findings from preclinical research on these two compounds. We discuss the compound identification, mechanism of action, drug resistance, in vitro activity, in vivo pharmacokinetic profiles, and preclinical in vivo activity and efficacy. Although delamanid and pretomanid share many similarities, several differences could be identified. One finding of particular interest is that certain Mycobacterium tuberculosis isolates have been described that are resistant to either delamanid or pretomanid, but with preserved susceptibility to the other compound. This might imply that delamanid and pretomanid could replace one another in certain regimens. Regarding bactericidal activity, based on in vitro and preclinical in vivo activity, delamanid has lower MICs and higher mycobacterial load reductions at lower drug concentrations and doses compared with pretomanid. However, when comparing in vivo preclinical bactericidal activity at dose levels equivalent to currently approved clinical doses based on drug exposure, this difference in activity between the two compounds fades. However, it is important to interpret these comparative results with caution knowing the variability inherent in preclinical in vitro and in vivo models.

Published

2022

8. GSK2556286 Is a Novel Antitubercular Drug Candidate Effective In Vivo with the Potential To Shorten Tuberculosis Treatment

Author

Eric L. Nuermberger, Maria Santos Martínez-Martínez, Olalla Sanz, Beatriz Urones, Jorge Esquivias, Heena Soni, Rokeya Tasneen, Sandeep Tyagi, Si-Yang Li, Paul J. Converse, Helena I. Boshoff, Gregory T. Robertson, Gurdyal S. Besra, Katherine A. Abrahams, Anna M. Upton, Khisimuzi Mdluli, Gary W. Boyle, Sam Turner, Nader Fotouhi, Nicholas C. Cammack, Juan Miguel Siles, Marta Alonso, Jaime Escribano, Joel Lelievre, Joaquin Rullas-Trincado, Esther Pérez-Herrán, Robert H. Bates, Gareth Maher-Edwards, David Barros, Lluís Ballell, and Elena Jiménez

Subjects

Pharmacology, Infectious Diseases, Pharmacology (medical)

Abstract

As a result of a high-throughput compound screening campaign using Mycobacterium tuberculosis -infected macrophages, a new drug candidate for the treatment of tuberculosis has been identified. GSK2556286 inhibits growth within human macrophages (50% inhibitory concentration [IC 50 ] = 0.07 μM), is active against extracellular bacteria in cholesterol-containing culture medium, and exhibits no cross-resistance with known antitubercular drugs.

Published

2022

9. Predictive Modeling to Study the Treatment-Shortening Potential of Novel Tuberculosis Drug Regimens, Toward Bundling of Preclinical Data

Author

Jurriaan E. M. de Steenwinkel, Rami Ayoun Alsoud, Hannelore I. Bax, Saskia E. Mudde, Manisha U. Lotlikar, Aart van der Meijden, Anna M. Upton, Ulrika S. H. Simonsson, Medical Microbiology & Infectious Diseases, and Internal Medicine

Subjects

Oncology, medicine.medical_specialty, Infectious Medicine, Tuberculosis, Antitubercular Agents, Infektionsmedicin, chemistry.chemical_compound, SDG 3 - Good Health and Well-being, Moxifloxacin, Internal medicine, pharmacodynamics, Immunology and Allergy, Medicine, Humans, Ethambutol, mouse, treatment duration, business.industry, Mycobacterium tuberculosis, Pyrazinamide, medicine.disease, Regimen, Infectious Diseases, chemistry, tuberculosis, Pretomanid, Drug Therapy, Combination, Bedaquiline, Rifampin, business, pharmacokinetics, Rifampicin, medicine.drug

Abstract

Background Given the persistently high global burden of tuberculosis, effective and shorter treatment options are needed. We explored the relationship between relapse and treatment length as well as interregimen differences for 2 novel antituberculosis drug regimens using a mouse model of tuberculosis infection and mathematical modeling. Methods Mycobacterium tuberculosis–infected mice were treated for up to 13 weeks with bedaquiline and pretomanid combined with moxifloxacin and pyrazinamide (BPaMZ) or linezolid (BPaL). Cure rates were evaluated 12 weeks after treatment completion. The standard regimen of isoniazid, rifampicin, pyrazinamide, and ethambutol (HRZE) was evaluated as a comparator. Results Six weeks of BPaMZ was sufficient to achieve cure in all mice. In contrast, 13 weeks of BPaL and 24 weeks of HRZE did not achieve 100% cure rates. Based on mathematical model predictions, 95% probability of cure was predicted to occur at 1.6, 4.3, and 7.9 months for BPaMZ, BPaL, and HRZE, respectively. Conclusion This study provides additional evidence for the treatment-shortening capacity of BPaMZ over BPaL and HRZE. To optimally use preclinical data for predicting clinical outcomes, and to overcome the limitations that hamper such extrapolation, we advocate bundling of available published preclinical data into mathematical models.

Published

2022

10. Comparative Efficacy of the Novel Diarylquinoline TBAJ-876 and Bedaquiline against a Resistant Rv0678 Mutant in a Mouse Model of Tuberculosis

Author

Deepak Almeida, Paul J. Converse, Si-Yang Li, Anna M. Upton, Nader Fotouhi, and Eric L. Nuermberger

Subjects

Pharmacology, Infectious Diseases, Pharmacology (medical)

Abstract

Bedaquiline (BDQ, B) is the first-in-class diarylquinoline to be approved for treatment of tuberculosis (TB). Recent guidelines recommend its use in treatment of multidrug- and extensively drug-resistant tuberculosis (MDR/XDR-TB).

Published

2021

11. Dual mTORC1/mTORC2 inhibition as a Host-Directed Therapeutic Target in Pathologically Distinct Mouse Models of Tuberculosis

Author

Anna M. Upton, Deborah S Mortensen, Natalie Hawryluk, Paul J. Converse, Nader Fotouhi, Eric L. Nuermberger, Rokeya Tasneen, and Michael E. Urbanowski

Subjects

isoniazid, pyrazinamide, Mechanistic Target of Rapamycin Complex 2, linezolid, mTORC1, Mechanistic Target of Rapamycin Complex 1, mTORC2, host-directed therapy, Mycobacterium tuberculosis, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Mediator, Immune system, Animals, Medicine, Experimental Therapeutics, Pharmacology (medical), bedaquiline, Protein Kinase Inhibitors, Ethambutol, PI3K/AKT/mTOR pathway, 030304 developmental biology, Pharmacology, 0303 health sciences, biology, Kinase, business.industry, Autophagy, biology.organism_classification, Infectious Diseases, tuberculosis, chemistry, Multiprotein Complexes, 030220 oncology & carcinogenesis, Pretomanid, pretomanid, Cancer research, Bedaquiline, business, rifampin, medicine.drug

Abstract

Efforts to develop more effective and shorter-course therapies for tuberculosis have included a focus on host-directed therapy (HDT). The goal of HDT is to modulate the host response to infection, thereby improving immune defenses to reduce the duration of antibacterial therapy and/or the amount of lung damage. As a mediator of innate and adaptive immune responses involved in eliminating intracellular pathogens, autophagy is a potential target for HDT in tuberculosis. Because Mycobacterium tuberculosis modulates mammalian target of rapamycin (mTOR) signaling to impede autophagy, pharmacologic mTOR inhibition could provide effective HDT. mTOR exists within two distinct multiprotein complexes, mTOR complex-1 (mTORC1) and mTOR complex-2 (mTORC2). Rapamycin and its analogs only partially inhibit mTORC1. We hypothesized that novel mTOR kinase inhibitors blocking both complexes would have expanded therapeutic potential. We compared the effects of two mTOR inhibitors: rapamycin and the orally available mTOR kinase domain inhibitor CC214-2, which blocks both mTORC1 and mTORC2, as adjunctive therapies against murine TB, when added to the first-line regimen (RHZE) or the novel bedaquiline-pretomanid-linezolid (BPaL) regimen. Neither mTOR inhibitor affected lung CFU counts after 4-8 weeks of treatment when combined with BPaL or RHZE. However, addition of CC214-2 to BPaL and RHZE was associated with significantly fewer relapses in C3HeB/FeJ compared to addition of rapamycin and, in RHZE-treated mice, resulted in fewer relapses compared to RHZE alone. Therefore, CC214-2 and related mTOR kinase inhibitors may be more effective candidates for HDT than rapamycin analogs and may have the potential to shorten the duration of TB treatment.

Published

2021

12. Synergistic Activity of Nitroimidazole-Oxazolidinone Conjugates against Anaerobic Bacteria

Author

Yu Lu, Zhuang Zhijun, Charles Z. Ding, Anthony Simon Lynch, Christopher B. Cooper, Wang Xiaomei, Ding Jun, William A. Denny, Zhenkun Ma, Ying Yuan, Wan Dawei, Qian Zhang, Anna M. Upton, and Shijie He

Subjects

Antitubercular Agents, Pharmaceutical Science, synergy, Drug resistance, Article, Analytical Chemistry, Microbiology, lcsh:QD241-441, Mycobacterium tuberculosis, 03 medical and health sciences, chemistry.chemical_compound, Bacteria, Anaerobic, 0302 clinical medicine, lcsh:Organic chemistry, Drug Resistance, Multiple, Bacterial, Drug Discovery, Tuberculosis, Multidrug-Resistant, Humans, nitroimidazole and oxazolidinone, Physical and Theoretical Chemistry, Oxazolidinones, 030304 developmental biology, 0303 health sciences, Nitroimidazole, biology, Bicyclic molecule, Organic Chemistry, Linezolid, Drug Synergism, Antimicrobial, biology.organism_classification, chemistry, Chemistry (miscellaneous), Nitroimidazoles, 030220 oncology & carcinogenesis, Pretomanid, drug conjugates, Molecular Medicine, anaerobic bacterium, Anaerobic bacteria

Abstract

The introductions of the bicyclic 4-nitroimidazole and the oxazolidinone classes of antimicrobial agents represented the most significant advancements in the infectious disease area during the past two decades. Pretomanid, a bicyclic 4-nitroimidazole, and linezolid, an oxazolidinone, are also part of a combination regimen approved recently by the US Food and Drug Administration for the treatment of pulmonary, extensively drug resistant (XDR), treatment-intolerant or nonresponsive multidrug-resistant (MDR) Mycobacterium tuberculosis (TB). To identify new antimicrobial agents with reduced propensity for the development of resistance, a series of dual-acting nitroimidazole-oxazolidinone conjugates were designed, synthesized and evaluated for their antimicrobial activity. Compounds in this conjugate series have shown synergistic activity against a panel of anaerobic bacteria, including those responsible for serious bacterial infections.

Published

2020

13. Synthetic Studies to Help Elucidate the Metabolism of the Preclinical Candidate TBAJ-876—A Less Toxic and More Potent Analogue of Bedaquiline

Author

Adrian Blaser, Amy S.T. Tong, Brian D. Palmer, Peter J. Choi, Daniel Conole, Hamish S. Sutherland, Anna M. Upton, William A. Denny, and Christopher B. Cooper

Subjects

Chemical Phenomena, Antitubercular Agents, Pharmaceutical Science, Chemistry Techniques, Synthetic, Pharmacology, 01 natural sciences, Analytical Chemistry, chemistry.chemical_compound, TMC207, Drug Discovery, Diarylquinolines, bedaquiline, media_common, 0303 health sciences, biology, Molecular Structure, Drug discovery, Drug development, tuberculosis, Chemistry (miscellaneous), Qtc interval prolongation, Molecular Medicine, Drug, Tuberculosis, media_common.quotation_subject, hERG, Article, lcsh:QD241-441, 03 medical and health sciences, lcsh:Organic chemistry, medicine, Animals, Humans, Physical and Theoretical Chemistry, 030304 developmental biology, mycobacterium tuberculosis, 010405 organic chemistry, business.industry, Spectrum Analysis, Organic Chemistry, TBAJ-876, Metabolism, medicine.disease, drug development, 0104 chemical sciences, Sirturo, chemistry, bedaquiline analogues, biology.protein, Bedaquiline, business

Abstract

Bedaquiline is a novel drug approved in 2012 by the FDA for treatment of drug-resistant tuberculosis (TB). Although it shows high efficacy towards drug-resistant forms of TB, its use has been limited by the potential for significant side effects. In particular, bedaquiline is a very lipophilic compound with an associated long terminal half-life and shows potent inhibition of the cardiac potassium hERG channel, resulting in QTc interval prolongation in humans that may result in cardiac arrhythmia. To address these issues, we carried out a drug discovery programme to develop an improved second generation analogue of bedaquiline. From this medicinal chemistry program, a candidate (TBAJ-876) has been selected to undergo further preclinical evaluation. During this evaluation, three major metabolites arising from TBAJ-876 were observed in several preclinical animal models. We report here our synthetic efforts to unequivocally structurally characterize these three metabolites through their independent directed synthesis.

Published

2020

14. TBAJ-876 Displays Bedaquiline-Like Mycobactericidal Potency without Retaining the Parental Drug’s Uncoupler Activity

Author

Gerhard Grüber, Jickky Palmae Sarathy, Priya Ragunathan, Christopher B. Cooper, Anna M. Upton, Thomas Dick, and School of Biological Sciences

Subjects

Drug, uncoupler, Bedaquiline, medicine.drug_class, Protonophore, media_common.quotation_subject, Lipid Bilayers, Antitubercular Agents, Microbial Sensitivity Tests, Pharmacology, Antimycobacterial, Electron Transport, 03 medical and health sciences, chemistry.chemical_compound, Adenosine Triphosphate, Diarylquinolines, medicine, Potency, Pharmacology (medical), bedaquiline, Mechanisms of Action: Physiological Effects, 030304 developmental biology, media_common, 0303 health sciences, ATP synthase, biology, Uncoupling Agents, 030306 microbiology, Chemistry, TBAJ-876, Mycobacterium tuberculosis, 3. Good health, Biological sciences::Molecular biology [Science], Infectious Diseases, tuberculosis, Mechanism of action, Biological sciences::Biochemistry [Science], biology.protein, protonophore, Protons, medicine.symptom

Abstract

The diarylquinoline F1FO-ATP synthase inhibitor bedaquiline (BDQ) displays protonophore activity. Thus, uncoupling electron transport from ATP synthesis appears to be a second mechanism of action of this antimycobacterial drug. Here, we show that the new BDQ analogue TBAJ-876 did not retain the parental drug’s protonophore activity. Comparative time-kill analyses revealed that both compounds exert the same bactericidal activity., The diarylquinoline F1FO-ATP synthase inhibitor bedaquiline (BDQ) displays protonophore activity. Thus, uncoupling electron transport from ATP synthesis appears to be a second mechanism of action of this antimycobacterial drug. Here, we show that the new BDQ analogue TBAJ-876 did not retain the parental drug’s protonophore activity. Comparative time-kill analyses revealed that both compounds exert the same bactericidal activity. These results suggest that the uncoupler activity is not required for the bactericidal activity of diarylquinolines.

Published

2020

15. Synthesis and structure-activity relationships for tetrahydroisoquinoline-based inhibitors of Mycobacterium tuberculosis

Author

Brian D. Palmer, Daniel Conole, Anna M. Upton, Peter J. Choi, Scott G. Franzblau, Hamish S. Sutherland, Amy S.T. Tong, Guo-Liang Lu, Manisha U. Lotlikar, Christopher B. Cooper, and William A. Denny

Subjects

Stereochemistry, Clinical Biochemistry, Antitubercular Agents, Pharmaceutical Science, Structure-activity relationships, Microbial Sensitivity Tests, 01 natural sciences, Biochemistry, Article, Mycobacterium tuberculosis, chemistry.chemical_compound, Synthesis, Structure-Activity Relationship, EtOAc, ethyl acetate, Tetrahydroisoquinolines, Drug Discovery, Side chain, DIPEA, N,N-diisopropylethylamine, Potency, Tuberculosis, Molecular Biology, ComputingMethodologies_COMPUTERGRAPHICS, biology, ATP synthase, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Tetrahydroisoquinoline, Organic Chemistry, Tetrahydroquinolines, biology.organism_classification, 0104 chemical sciences, DCM, dichloromethane, 010404 medicinal & biomolecular chemistry, chemistry, Et2O, diethyl ether, Lipophilicity, biology.protein, Microsome, Molecular Medicine, Bedaquiline, MeOH, methanol, THF, tetrahydrofuran

Abstract

Graphical abstract, A series of 5,8-disubstituted tetrahydroisoquinolines were shown to be effective inhibitors of M. tb in culture and modest inhibitors of M. tb ATP synthase. There was a broad general trend of improved potency with higher lipophilicity. Large substituents (e.g., Bn) at the tetrahydroquinoline 5-position were well-tolerated, while N-methylpiperazine was the preferred 8-substituent. Structure-activity relationships for 7-linked side chains showed that the nature of the 7-linking group was important; –CO– and –COCH2– linkers were less effective than –CH2– or –CONH– ones. This suggests that the positioning of a terminal aromatic ring is important for target binding. Selected compounds showed much faster rates of microsomal clearance than did the clinical ATP synthase inhibitor bedaquiline, and modest inhibition of mycobacterial ATP synthase.

Published

2020

16. Synthesis and structure-activity relationships for a new class of tetrahydronaphthalene amide inhibitors of Mycobacterium tuberculosis

Author

Hamish S. Sutherland, Guo-Liang Lu, Amy S.T. Tong, Daniel Conole, Scott G. Franzblau, Anna M. Upton, Manisha U. Lotlikar, Christopher B. Cooper, Brian D. Palmer, Peter J. Choi, and William A. Denny

Subjects

Pharmacology, Tetrahydronaphthalenes, Organic Chemistry, Antitubercular Agents, Microbial Sensitivity Tests, Mycobacterium tuberculosis, General Medicine, Amides, Mice, Structure-Activity Relationship, Liver, Drug Discovery, Animals, Humans, Diarylquinolines

Abstract

Drug resistant tuberculsosis (TB) is global health crisis that demands novel treatment strategies. Bacterial ATP synthase inhibitors such as bedaquiline and next-generation analogues (such as TBAJ-876) have shown promising efficacy in patient populations and preclinical studies, respectively, suggesting that selective targeting of this enzyme presents a validated therapeutic strategy for the treatment of TB. In this work, we report tetrahydronaphthalene amides (THNAs) as a new class of ATP synthase inhibitors that are effective in preventing the growth of Mycobacterium tuberculosis (M.tb) in culture. Design, synthesis and comprehensive structure-activity relationship studies for approximately 80 THNA analogues are described, with a small selection of compounds exhibiting potent (in some cases MIC

Published

2022

17. Variations in the C-unit of bedaquiline provides analogues with improved biology and pharmacology

Author

Peter J. Choi, William A. Denny, Hamish S. Sutherland, Adrian Blaser, Scott G. Franzblau, Christopher B. Cooper, Manisha U. Lotlikar, Amy S.T. Tong, Anna M. Upton, and Brian D. Palmer

Subjects

Drug, media_common.quotation_subject, Clinical Biochemistry, hERG, Antitubercular Agents, Pharmaceutical Science, Microbial Sensitivity Tests, Pharmacology, Biochemistry, chemistry.chemical_compound, Structure-Activity Relationship, In vivo, Drug Discovery, Potency, Animals, Humans, Diarylquinolines, Molecular Biology, media_common, biology, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Organic Chemistry, Mycobacterium tuberculosis, In vitro, Potassium channel, Lipophilicity, biology.protein, Molecular Medicine, Bedaquiline

Abstract

Analogues of the anti-tuberculosis drug bedaquiline, bearing a 3,5-dimethoxy-4-pyridyl C-unit, retain high anti-bacterial potency yet exert less inhibition of the hERG potassium channel, in vitro, than the parent compound. Two of these analogues (TBAJ-587 and TBAJ-876) are now in preclinical development. The present study further explores structure-activity relationships across a range of related 3,5-disubstituted-4-pyridyl C-unit bedaquiline analogues of greatly varying lipophilicity (clogP from 8.16 to 1.89). This broader class shows similar properties to the 3,5-dimethoxy-4-pyridyl series, being substantially more potent in vitro and equally active in an in vivo (mouse) model than bedaquiline, while retaining a lower cardiovascular risk profile through greatly attenuated hERG inhibition.

Published

2019

18. TBAJ-876 Retains Bedaquiline’s Activity against Subunits c and ε of Mycobacterium tuberculosis F-ATP Synthase

Author

Priya Ragunathan, Christopher B. Cooper, Thomas Dick, Joon Shin, Jickky Palmae Sarathy, Anna M. Upton, Gerhard Grüber, and School of Biological Sciences

Subjects

Protein Conformation, Protein subunit, Mutant, Antitubercular Agents, F-ATP Synthase, ε subunit, F-ATP synthase, 03 medical and health sciences, chemistry.chemical_compound, Bacterial Proteins, medicine, Pharmacology (medical), Binding site, bedaquiline, Diarylquinolines, Mode of action, Mechanisms of Action: Physiological Effects, 030304 developmental biology, Pharmacology, chemistry.chemical_classification, ε Subunit, 0303 health sciences, c subunit, ATP synthase, biology, 030306 microbiology, Chemistry, TBAJ-876, Mycobacterium tuberculosis, diarylquinoline, Molecular biology, 3. Good health, Protein Subunits, Proton-Translocating ATPases, Infectious Diseases, Enzyme, Biological sciences::Molecular biology [Science], Mechanism of action, Biological sciences::Biochemistry [Science], biology.protein, medicine.symptom, Bedaquiline

Abstract

The antituberculosis drug bedaquiline (BDQ) inhibits Mycobacterium tuberculosis F-ATP synthase by interfering with two subunits. Drug binding to the c subunit stalls the rotation of the c ring, while binding to the ε subunit blocks coupling of c ring rotation to ATP synthesis at the catalytic α3:β3 headpiece. BDQ is used for the treatment of drug-resistant tuberculosis., The antituberculosis drug bedaquiline (BDQ) inhibits Mycobacterium tuberculosis F-ATP synthase by interfering with two subunits. Drug binding to the c subunit stalls the rotation of the c ring, while binding to the ε subunit blocks coupling of c ring rotation to ATP synthesis at the catalytic α3:β3 headpiece. BDQ is used for the treatment of drug-resistant tuberculosis. However, the drug is highly lipophilic, displays a long terminal half-life, and has a cardiotoxicity liability by causing QT interval prolongation. Recent medicinal chemistry campaigns have resulted in the discovery of 3,5-dialkoxypyridine analogues of BDQ that are less lipophilic, have higher clearance, and display lower cardiotoxic potential. TBAJ-876, which is a new developmental compound of this series, shows attractive antitubercular activity and efficacy in a murine tuberculosis model. Here, we asked whether TBAJ-876 and selected analogues of the compound retain BDQ’s mechanism of action. Biochemical assays showed that TBAJ-876 is a potent inhibitor of mycobacterial F-ATP synthase. Selection of spontaneous TBAJ-876-resistant mutants identified missense mutations at BDQ’s binding site on the c subunit, suggesting that TBAJ-876 retains BDQ’s targeting of the c ring. Susceptibility testing against a strain overexpressing the ε subunit and a strain harboring an engineered mutation in BDQ’s ε subunit binding site suggest that TBAJ-876 retains BDQ’s activity on the ε subunit. Nuclear magnetic resonance (NMR) titration studies confirmed that TBAJ-876 binds to the ε subunit at BDQ’s binding site. We show that TBAJ-876 retains BDQ’s antimycobacterial mode of action. The developmental compound inhibits the mycobacterial F-ATP synthase via a dual-subunit mechanism of interfering with the functions of both the enzyme’s c and ε subunits.

Published

2019

19. Structure-activity relationships for unit C pyridyl analogues of the tuberculosis drug bedaquiline

Author

Hamish S. Sutherland, Peter J. Choi, Scott G. Franzblau, Christopher B. Cooper, Daniel Conole, Manisha U. Lotlikar, Brian D. Palmer, William A. Denny, Anna M. Upton, Adrian Blaser, and Amy S.T. Tong

Subjects

Drug, Tuberculosis, Pyridines, media_common.quotation_subject, Clinical Biochemistry, hERG, Antitubercular Agents, Pharmaceutical Science, Microbial Sensitivity Tests, Pharmacology, 01 natural sciences, Biochemistry, Article, chemistry.chemical_compound, Mice, Structure-Activity Relationship, In vivo, Drug Discovery, medicine, Potassium Channel Blockers, Potency, Animals, Humans, Diarylquinolines, Molecular Biology, media_common, biology, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Organic Chemistry, Mycobacterium tuberculosis, medicine.disease, Potassium channel, Ether-A-Go-Go Potassium Channels, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, chemistry, Lipophilicity, biology.protein, Molecular Medicine, Bedaquiline

Abstract

The ATP-synthase inhibitor bedaquiline is effective against drug-resistant tuberculosis but is extremely lipophilic (clogP 7.25) with a very long plasma half-life. Additionally, inhibition of potassium current through the cardiac hERG channel by bedaquiline, is associated with prolongation of the QT interval, necessitating cardiovascular monitoring. Analogues were prepared where the naphthalene C-unit was replaced with substituted pyridines to produce compounds with reduced lipophilicity, anticipating a reduction in half-life. While there was a direct correlation between in vitro inhibitory activity against M. tuberculosis (MIC(90)) and compound lipophilicity, potency only fell off sharply below a clogP of about 4.0, providing a useful lower bound for analogue design. The bulk of the compounds remained potent inhibitors of the hERG potassium channel, with notable exceptions where IC(50) values were at least 5-fold higher than that of bedaquiline. Many of the compounds had desirably higher rates of clearance than bedaquiline, but this was associated with lower plasma exposures in mice, and similar or higher MICs resulted in lower AUC/MIC ratios than bedaquiline for most compounds. The two compounds with lower potency against hERG exhibited similar clearance to bedaquiline and excellent efficacy in vivo, suggesting further exploration of C-ring pyridyls is worthwhile.

Published

2019

20. Contribution of Pretomanid to Novel Regimens Containing Bedaquiline with either Linezolid or Moxifloxacin and Pyrazinamide in Murine Models of Tuberculosis

Author

Jian, Xu, Si-Yang, Li, Deepak V, Almeida, Rokeya, Tasneen, Kala, Barnes-Boyle, Paul J, Converse, Anna M, Upton, Khisimuzi, Mdluli, Nader, Fotouhi, and Eric L, Nuermberger

Subjects

Mice, Inbred BALB C, pyrazinamide, Moxifloxacin, Antitubercular Agents, Linezolid, Mice, Nude, murine model, resistance, Disease Models, Animal, Mice, Nitroimidazoles, RNA, Ribosomal, 16S, pretomanid, Animals, Tuberculosis, Female, Experimental Therapeutics, Diarylquinolines, bedaquiline

Abstract

Novel regimens combining bedaquiline and pretomanid with either linezolid (BPaL regimen) or moxifloxacin and pyrazinamide (BPaMZ regimen) shorten the treatment duration needed to cure tuberculosis (TB) in BALB/c mice compared to that of the first-line regimen and have yielded promising results in initial clinical trials. However, the independent contribution of the investigational new drug pretomanid to the efficacy of BPaMZ has not been examined, and its contribution to BPaL has been examined only over the first 2 months of treatment., Novel regimens combining bedaquiline and pretomanid with either linezolid (BPaL regimen) or moxifloxacin and pyrazinamide (BPaMZ regimen) shorten the treatment duration needed to cure tuberculosis (TB) in BALB/c mice compared to that of the first-line regimen and have yielded promising results in initial clinical trials. However, the independent contribution of the investigational new drug pretomanid to the efficacy of BPaMZ has not been examined, and its contribution to BPaL has been examined only over the first 2 months of treatment. In the present study, the addition of pretomanid to BL increased bactericidal activity, prevented emergence of bedaquiline resistance, and shortened the duration needed to prevent relapse with drug-susceptible isolates by at least 2 months in BALB/c mice. Addition of pretomanid to bedaquiline, moxifloxacin, and pyrazinamide (BMZ) resulted in a 1-log10 greater CFU reduction after 1 month of treatment and/or reduced the number of mice relapsing in each of 2 experiments in BALB/c mice and in immunocompromised nude mice. Bedaquiline-resistant isolates were found at relapse in only one BMZ-treated nude mouse. Treatment of infection with a pyrazinamide-resistant mutant in BALB/c mice with BPaMZ prevented selection of bedaquiline-resistant mutants and reduced the proportion of mice relapsing compared to that for BMZ treatment alone. Among severely ill C3HeB/FeJ mice with caseous pneumonia and cavitation, BPaMZ increased median survival (≥60 versus 21 days) and reduced median lung CFU by 2.4 log10 at 1 month compared to the level for BMZ. In conclusion, in 3 different mouse models, pretomanid contributed significantly to the efficacy of the BPaMZ and BPaL regimens, including restricting the selection of bedaquiline-resistant mutants.

Published

2019

21. 3,5-Dialkoxypyridine analogues of bedaquiline are potent antituberculosis agents with minimal inhibition of the hERG channel

Author

William A. Denny, Peter J. Choi, Scott G. Franzblau, Christopher B. Cooper, Adrian Blaser, Brian D. Palmer, Daniel Conole, Amy S.T. Tong, Anna M. Upton, Hamish S. Sutherland, and Manisha U. Lotlikar

Subjects

Tuberculosis, Pyridines, Clinical Biochemistry, hERG, Antitubercular Agents, Pharmaceutical Science, Microbial Sensitivity Tests, Pharmacology, 01 natural sciences, Biochemistry, QT interval, Article, chemistry.chemical_compound, Structure-Activity Relationship, In vivo, Drug Discovery, medicine, Potassium Channel Blockers, Humans, Diarylquinolines, Molecular Biology, biology, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Chemistry, Organic Chemistry, Mycobacterium tuberculosis, medicine.disease, Potassium channel, Ether-A-Go-Go Potassium Channels, 0104 chemical sciences, Blockade, 010404 medicinal & biomolecular chemistry, Lipophilicity, biology.protein, Molecular Medicine, Bedaquiline

Abstract

Bedaquiline is a new drug of the diarylquinoline class that has proven to be clinically effective against drug-resistant tuberculosis, but has a cardiac liability (prolongation of the QT interval) due to its potent inhibition of the cardiac potassium channel protein hERG. Bedaquiline is highly lipophilic and has an extremely long terminal half-life, so has the potential for more-than-desired accumulation in tissues during the relatively long treatment durations required to cure TB. The present work is part of a program that seeks to identify a diarylquinoline that is as potent as bedaquiline against Mycobacterium tuberculosis, with lower lipophilicity, higher clearance, and lower risk for QT prolongation. Previous work led to the identification of compounds with greatly-reduced lipophilicity compounds that retain good anti-tubercular activity in vitro and in mouse models of TB, but has not addressed the hERG blockade. We now present compounds where the C-unit naphthalene is replaced by a 3,5-dialkoxy-4-pyridyl, demonstrate more potent in vitro and in vivo anti-tubercular activity, with greatly attenuated hERG blockade. Two examples of this series are in preclinical development.

Published

2018

22. Structure-activity relationships for analogs of the tuberculosis drug bedaquiline with the naphthalene unit replaced by bicyclic heterocycles

Author

Hamish S, Sutherland, Amy S T, Tong, Peter J, Choi, Daniel, Conole, Adrian, Blaser, Scott G, Franzblau, Christopher B, Cooper, Anna M, Upton, Manisha U, Lotlikar, William A, Denny, and Brian D, Palmer

Subjects

Dose-Response Relationship, Drug, Molecular Structure, Bedaquiline, Antitubercular Agents, Drug development, Microbial Sensitivity Tests, Mycobacterium tuberculosis, Naphthalenes, Bridged Bicyclo Compounds, Heterocyclic, Bedaquiline analogs, Article, Structure-Activity Relationship, Cell Line, Tumor, Humans, Tuberculosis, Diarylquinolines, ComputingMethodologies_COMPUTERGRAPHICS

Abstract

Graphical abstract, Replacing the naphthalene C-unit of the anti-tuberculosis drug bedaquiline with a range of bicyclic heterocycles of widely differing lipophilicity gave analogs with a 4.5-fold range in clogP values. The biological results for these compounds indicate on average a lower clogP limit of about 5.0 in this series for retention of potent inhibitory activity (MIC90s) against M.tb in culture. Some of the compounds also showed a significant reduction in inhibition of hERG channel potassium current compared with bedaquiline, but there was no common structural feature that distinguished these.

Published

2017

23. Identification and optimization of a new series of anti-tubercular quinazolinones

Author

Jerome Menegotto, Cédric Couturier, Anna M. Upton, Christine Lair, Eric Bacqué, Sophie Lagrange, Armin Bauer, Takushi Kaneko, Bodo Scheiper, Eric Cogo, Corinne Perron, and Alain Pellet

Subjects

0301 basic medicine, Tuberculosis, Phenotypic screening, High-throughput screening, 030106 microbiology, Clinical Biochemistry, Mycobacterium smegmatis, Antitubercular Agents, Pharmaceutical Science, Microbial Sensitivity Tests, Pharmacology, Biochemistry, Cell Line, 03 medical and health sciences, Mice, Structure-Activity Relationship, In vivo, Drug Discovery, medicine, Extracellular, Potency, Animals, Humans, Molecular Biology, Quinazolinones, biology, Chemistry, Organic Chemistry, Mycobacterium tuberculosis, medicine.disease, biology.organism_classification, In vitro, High-Throughput Screening Assays, 030104 developmental biology, Molecular Medicine

Abstract

A high throughput phenotypic screening against Mycobacterium smegmatis led us to the discovery of a new class of bacteriostatic, highly hydrophobic antitubercular quinazolinones that potently inhibited the in vitro growth of either extracellular or intramacrophagic M. tuberculosis (Mtb), via modulation of an unidentified but yet novel target. Optimization of the initial hit compound culminated in the identification of potent but poorly soluble Mtb growth inhibitors, three of which were progressed to in vivo efficacy studies. Despite nanomolar in vitro potency and attractive PK properties, none of these compounds was convincingly potent in our in vivo mouse tuberculosis models. This lack of efficacy may be linked to the poor drug-likeness of the test molecules and/or to the properties of the target.

Published

2016

24. In Vitro and In Vivo Activities of the Nitroimidazole TBA-354 against Mycobacterium tuberculosis

Author

Khisimuzi Mdluli, B. Wang, Yu Lu, Jian Xu, Y. Kim, Yijin Wang, Zhenkun Ma, Anna M. Upton, T. J. Yang, Scott G. Franzblau, and Sang-Hyun Cho

Subjects

Tuberculosis, Antitubercular Agents, Microbial Sensitivity Tests, Biology, Pharmacology, Mycobacterium tuberculosis, chemistry.chemical_compound, Mice, In vivo, Cell Line, Tumor, Drug Resistance, Bacterial, Oxazines, medicine, Potency, Animals, Humans, Pharmacology (medical), Experimental Therapeutics, Drug Interactions, Oxazoles, Mice, Inbred BALB C, Nitroimidazole, biology.organism_classification, medicine.disease, In vitro, Bioavailability, Disease Models, Animal, Infectious Diseases, chemistry, Nitroimidazoles, Female, Delamanid, Caco-2 Cells, medicine.drug

Abstract

Nitroimidazoles are a promising new class of antitubercular agents. The nitroimidazo-oxazole delamanid (OPC-67683, Deltyba) is in phase III trials for the treatment of multidrug-resistant tuberculosis, while the nitroimidazo-oxazine PA-824 is entering phase III for drug-sensitive and drug-resistant tuberculosis. TBA-354 (SN31354[( S )-2-nitro-6-((6-(4-trifluoromethoxy)phenyl)pyridine-3-yl)methoxy)-6,7-dihydro-5 H -imidazo[2,1- b ][1,3]oxazine]) is a pyridine-containing biaryl compound with exceptional efficacy against chronic murine tuberculosis and favorable bioavailability in preliminary rodent studies. It was selected as a potential next-generation antituberculosis nitroimidazole following an extensive medicinal chemistry effort. Here, we further evaluate the pharmacokinetic properties and activity of TBA-354 against Mycobacterium tuberculosis . TBA-354 is narrow spectrum and bactericidal in vitro against replicating and nonreplicating Mycobacterium tuberculosis , with potency similar to that of delamanid and greater than that of PA-824. The addition of serum protein or albumin does not significantly alter this activity. TBA-354 maintains activity against Mycobacterium tuberculosis H37Rv isogenic monoresistant strains and clinical drug-sensitive and drug-resistant isolates. Spontaneous resistant mutants appear at a frequency of 3 × 10 −7 . In vitro studies and in vivo studies in mice confirm that TBA-354 has high bioavailability and a long elimination half-life. In vitro studies suggest a low risk of drug-drug interactions. Low-dose aerosol infection models of acute and chronic murine tuberculosis reveal time- and dose-dependent in vivo bactericidal activity that is at least as potent as that of delamanid and more potent than that of PA-824. Its superior potency and pharmacokinetic profile that predicts suitability for once-daily oral dosing suggest that TBA-354 be studied further for its potential as a next-generation nitroimidazole.

Published

2014

25. Design, synthesis, and structure-activity relationship studies of tryptanthrins as antitubercular agents

Author

Takushi Kaneko, Zhenkun Ma, Anna M. Upton, Pilho Kim, Sang Nae Cho, Scott G. Franzblau, Taegwon Oh, and Jae Min Hwang

Subjects

Antitubercular Agents, Pharmaceutical Science, Microbial Sensitivity Tests, Pharmacology, Biology, Analytical Chemistry, Mycobacterium tuberculosis, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Pharmacokinetics, Cytochrome P-450 Enzyme System, In vivo, Drug Discovery, Structure–activity relationship, Animals, Humans, Tuberculosis, ADME, Natural product, Molecular Structure, Organic Chemistry, biology.organism_classification, In vitro, Bioavailability, Rats, Mice, Inbred C57BL, Complementary and alternative medicine, chemistry, Drug Design, Quinazolines, Molecular Medicine

Abstract

The natural product tryptanthrin (1a) represents a potential lead for new tuberculosis (TB) drugs since tryptanthrin and its synthetic analogues possess potent in vitro activity against Mycobacterium tuberculosis (Mtb). However, in spite of their in vitro activity, none of these agents have been shown to be efficacious in vivo against animal models of TB. Described herein are syntheses of new tryptanthrin analogues together with a systematic investigation of their in vitro antitubercular activity and ADME properties followed by pharmacokinetic characterization in rodents for the most promising compounds. Those with the best potency and oral bioavailability were progressed to evaluations of efficacy against acute murine TB. The work aimed to prove the concept that this compound class can limit growth of Mtb during infection as well as to establish the SAR for in vitro activity against Mtb and the range of in vitro ADME parameters for this class of natural products. Novel C-11-deoxy (5b) and A-ring-saturated (6) tryptanthrin analogues were discovered that maintained activity against Mtb and showed improved solubility compared to tryptanthrin as well as evidence of oral bioavailability in rodents. However, neither 5b nor 6 demonstrated efficacy against acute murine TB following administration at doses up to 400 mg/kg daily for 4 weeks. Although 5b and 6 failed to inhibit replication or kill Mtb in vivo, they illuminate a path to new structural variations of the tryptanthrin scaffold that may maximize the potential of this class of compounds against TB.

Published

2013

26. Identification of less lipophilic riminophenazine derivatives for the treatment of drug-resistant tuberculosis

Author

Jingbin Wang, Kai Liu, Yanyan Hou, Yu Lu, Yang Liu, Ningbo Gong, Christopher B. Cooper, Yang Lv, Bin Wang, Binna Liu, Dali Yin, Zhenkun Ma, Anna M. Upton, Lei Fu, Gang Zhang, Haihong Huang, Li Chun, Dongfeng Zhang, Meiqin Zheng, and Hao Zhang

Subjects

Male, Tuberculosis, Antitubercular Agents, Drug resistance, Microbial Sensitivity Tests, Pharmacology, Crystallography, X-Ray, Clofazimine, Mycobacterium tuberculosis, Mice, Structure-Activity Relationship, In vivo, Drug Resistance, Multiple, Bacterial, Drug Discovery, Tuberculosis, Multidrug-Resistant, medicine, Toxicity Tests, Acute, Animals, Cytotoxicity, Mice, Inbred BALB C, biology, Molecular Structure, Chemistry, biology.organism_classification, medicine.disease, Multiple drug resistance, Lipophilicity, Molecular Medicine, medicine.drug

Abstract

Clofazimine (CFZ), a member of the riminophenazine class, has been studied in clinical trials for the treatment of multidrug-resistant tuberculosis (MDR-TB). CFZ has several side effects which can be attributed to its extremely high lipophilicity. A series of novel riminophenazine analogues bearing a C-2 pyridyl substituent was designed and synthesized with the goal of maintaining potent activity against Mycobacterium tuberculosis (M. tuberculosis) while improving upon its safety profile by lowering the lipophilicity. All compounds were evaluated for their in vitro activity and cytotoxicity. The results demonstrated that many new compounds had potent activity against M. tuberculosis with MICs of less than 0.03 μg/mL and low cytotoxicity with IC(50) values greater than 64 μg/mL. Some compounds were tested for in vivo efficacy against MDR-TB in an experimental mouse infection model. Two compounds demonstrated equivalent or better efficacy than CFZ in this model with significantly reduced skin discoloration potential.

Published

2012

27. Clofazimine Analogs with Efficacy against Experimental Tuberculosis and Reduced Potential for Accumulation▿

Author

Haixia Jin, Lei Fu, Anna M. Upton, Bin Wang, Zhenkun Ma, Yu Lu, Jian Xu, Weijie Zhao, Haihong Huang, Hui Zhu, Peng Li, Dali Yin, and Meiqin Zheng

Subjects

Male, Tuberculosis, Antitubercular Agents, Administration, Oral, Microbial Sensitivity Tests, Pharmacology, Clofazimine, Cell Line, Mycobacterium tuberculosis, Mice, Pharmacotherapy, Pharmacokinetics, Chlorocebus aethiops, medicine, Animals, Pharmacology (medical), Experimental Therapeutics, Mode of action, Vero Cells, Mice, Inbred BALB C, biology, business.industry, biology.organism_classification, medicine.disease, Infectious Diseases, Drug development, Leprosy, business, medicine.drug

Abstract

The global tuberculosis crisis urgently demands new, efficacious, orally available drugs with the potential to shorten and simplify the long and complex treatments for drug-sensitive and drug-resistant disease. Clofazimine, a riminophenazine used for many years to treat leprosy, demonstrates efficacy in animal models of tuberculosis via a novel mode of action. However, clofazimine's physicochemical and pharmacokinetic properties contribute to side effects that limit its use; in particular, an extremely long half-life and propensity for tissue accumulation together with clofazimine's dye properties leads to unwelcome skin discoloration. We recently conducted a systematic structure-activity study of more than 500 riminophenazine analogs for anti- Mycobacterium tuberculosis activity. We describe here the characteristics of 12 prioritized compounds in more detail. The new riminophenazine analogs demonstrated enhanced in vitro activity compared to clofazimine against replicating M. tuberculosis H37Rv, as well as panels of drug-sensitive and drug-resistant clinical isolates. The new compounds demonstrate at least equivalent activity compared to clofazimine against intracellular M. tuberculosis and, in addition, most of them were active against nonreplicating M. tuberculosis . Eleven of these more water-soluble riminophenazine analogs possess shorter half-lives than clofazimine when dosed orally to mice, suggesting that they may accumulate less. Most importantly, the nine compounds that progressed to efficacy testing demonstrated inhibition of bacterial growth in the lungs that is superior to the activity of an equivalent dose of clofazimine when administered orally for 20 days in a murine model of acute tuberculosis. The efficacy of these compounds, along with their decreased potential for accumulation and therefore perhaps also for tissue discoloration, warrants further study.

Published

2011

28. Role of the methylcitrate cycle in propionate metabolism and detoxification in Mycobacterium smegmatis

Author

John D. McKinney and Anna M. Upton

Subjects

Mycobacterium smegmatis, Glyoxylate cycle, Methylisocitrate lyase, Microbiology, Citric Acid, Mice, Bacterial Proteins, Animals, Carbon-Carbon Lyases, chemistry.chemical_classification, biology, Catabolism, Genetic Complementation Test, Computational Biology, Mycobacterium tuberculosis, Metabolism, Isocitrate lyase, biology.organism_classification, Isocitrate Lyase, Culture Media, Isoenzymes, chemistry, Biochemistry, Dehydratase, Propionate, Transformation, Bacterial, Propionates, Gene Deletion

Abstract

Catabolism of odd-chain-length fatty acids yields acetyl-CoA and propionyl-CoA. A common pathway of propionyl-CoA metabolism in micro-organisms is the methylcitrate cycle, which includes the dedicated enzymes methylcitrate synthase (MCS), methylcitrate dehydratase (MCD) and methylisocitrate lyase (MCL). The methylcitrate cycle is essential for propionate metabolism in Mycobacterium tuberculosis. Unusually, M. tuberculosis lacks an MCL orthologue and this activity is provided instead by two isoforms of the glyoxylate cycle enzyme isocitrate lyase (ICL1 and ICL2). These bifunctional (ICL/MCL) enzymes are jointly required for propionate metabolism and for growth and survival in mice. In contrast, the non-pathogenic species Mycobacterium smegmatis encodes a canonical MCL enzyme in addition to ICL1 and ICL2. The M. smegmatis gene encoding MCL (prpB) is clustered with genes encoding MCS (prpC) and MCD (prpD). Here we show that deletion of the M. smegmatis prpDBC locus reduced but did not eliminate MCL activity in cell-free extracts. The residual MCL activity was abolished by deletion of icl1 and icl2 in the DeltaprpDBC background, suggesting that these genes encode bifunctional ICL/MCL enzymes. A DeltaprpB Deltaicl1 Deltaicl2 mutant was unable to grow on propionate or mixtures of propionate and glucose. We hypothesize that incomplete propionyl-CoA metabolism might cause toxic metabolites to accumulate. Consistent with this idea, deletion of prpC and prpD in the DeltaprpB Deltaicl1 Deltaicl2 background paradoxically restored growth on propionate-containing media. These observations suggest that the marked attenuation of ICL1/ICL2-deficient M. tuberculosis in mice could be due to the accumulation of toxic propionyl-CoA metabolites, rather than inability to utilize fatty acids per se.

29. Role of the methylcitrate cycle in Mycobacterium tuberculosis metabolism, intracellular growth, and virulence

Author

Ernesto J. Muñoz-Elías, Anna M. Upton, John D. McKinney, and Joseph Cherian

Subjects

Male, Molecular Sequence Data, Glyoxylate cycle, Bone Marrow Cells, Methylisocitrate lyase, Citrate (si)-Synthase, Microbiology, Citric Acid, Mycobacterium tuberculosis, Mice, Animals, Carbon-Carbon Lyases, Molecular Biology, Cells, Cultured, Hydro-Lyases, Phylogeny, chemistry.chemical_classification, Molecular Structure, biology, Escherichia coli Proteins, Macrophages, Fatty acid, Isocitrate lyase, Metabolism, biology.organism_classification, Isocitrate Lyase, Isoenzymes, Mice, Inbred C57BL, Complementation, Biochemistry, chemistry, Female, Propionates, Bacteria

Abstract

Growth of bacteria and fungi on fatty acid substrates requires the catabolic beta-oxidation cycle and the anaplerotic glyoxylate cycle. Propionyl-CoA generated by beta-oxidation of odd-chain fatty acids is metabolized via the methylcitrate cycle. Mycobacterium tuberculosis possesses homologues of methylcitrate synthase (MCS) and methylcitrate dehydratase (MCD) but not 2-methylisocitrate lyase (MCL). Although MCLs share limited homology with isocitrate lyases (ICLs) of the glyoxylate cycle, these enzymes are thought to be functionally non-overlapping. Previously we reported that the M. tuberculosis ICL isoforms 1 and 2 are jointly required for growth on fatty acids, in macrophages, and in mice. ICL-deficient bacteria could not grow on propionate, suggesting that in M. tuberculosis ICL1 and ICL2 might function as ICLs in the glyoxylate cycle and as MCLs in the methylcitrate cycle. Here we provide biochemical and genetic evidence supporting this interpretation. The role of the methylcitrate cycle in M. tuberculosis metabolism was further evaluated by constructing a mutant strain in which prpC (encoding MCS) and prpD (encoding MCD) were deleted. The DeltaprpDC strain could not grow on propionate media in vitro or in murine bone marrow-derived macrophages infected ex vivo; growth under these conditions was restored by complementation with a plasmid containing prpDC. Paradoxically, bacterial growth and persistence, and tissue pathology, were indistinguishable in mice infected with wild-type or DeltaprpDC bacteria.