GaMF1.39’s antibiotic efficacy and its enhanced antitubercular activity in combination with clofazimine, Telacebec, ND-011992, or TBAJ-876-Reference-Cited by-同舟云学术

GaMF1.39’s antibiotic efficacy and its enhanced antitubercular activity in combination with clofazimine, Telacebec, ND-011992, or TBAJ-876

Published:2023-12-12 Issue:6 Volume:11 Page:
ISSN:2165-0497
Container-title:Microbiology Spectrum
language:en
Short-container-title:Microbiol Spectr

Author:

Ragunathan Priya¹^ORCID,Shuyi Ng Pearly²,Singh Samsher³^ORCID,Poh Wee Han⁴,Litty Dennis⁵,Kalia Nitin Pal⁶^ORCID,Larsson Simon³,Harikishore Amaravadhi¹⁷^ORCID,Rice Scott A.¹⁴,Ingham Philip W.³^ORCID,Müller Volker⁵^ORCID,Moraski Garrett⁸^ORCID,Miller Marvin J.⁹^ORCID,Dick Thomas¹⁰¹¹¹²^ORCID,Pethe Kevin¹³¹³^ORCID,Grüber Gerhard¹^ORCID

Affiliation:

1. School of Biological Sciences, Nanyang Technological University , Singapore, Singapore

2. Experimental Drug Development Centre, Agency for Science, Technology and Research , Singapore, Singapore

3. Lee Kong Chian School of Medicine, Nanyang Technological University, Experimental Medicine Building , Singapore, Singapore

4. Singapore Centre for Environmental Life Sciences Engineering, Nanyang Technological University , Singapore, Singapore

5. Molecular Microbiology and Bioenergetics, Institute for Molecular Biosciences, Johann Wolfgang Goethe University Frankfurt/Main , Frankfurt, Germany

6. Department of Biological Sciences (Pharmacology & Toxicology), National Institute of Pharmaceutical Education and Research , Hyderabad, Telangana, India

7. School of Chemistry, Chemical Engineering and Biotechnology, Nanyang Technological University , Singapore, Singapore

8. Department of Chemistry and Biochemistry, Montana State University , Bozeman, Montana, USA

9. Department of Chemistry and Biochemistry, University of Notre Dame , Notre Dame, Indiana, USA

10. Center for Discovery and Innovation, Hackensack Meridian Health , Nutley, New Jersey, USA

11. Department of Medical Sciences, Hackensack Meridian School of Medicine , Nutley, New Jersey, USA

12. Department of Microbiology and Immunology, Georgetown University , Washington, DC, USA

13. National Centre for Infectious Diseases (NCID), Jalan Tan Tock Seng , Singapore, Singapore

Abstract

ABSTRACT The Mycobacterium tuberculosis ( Mtb ) F-ATP synthase generates most of the biological energy currency ATP. Previously, we identified the mycobacterium-specific loop of the F-ATP synthase subunit γ as a new anti-tuberculosis target and discovered the novel diaminopyrimidine GaMF1, whose potency was improved by structure-activity relationship studies leading to the analog GaMF1.39. Here, we report that GaMF1.39 depletes cellular ATP formation by targeting the mycobacterial F-ATP synthase without affecting proton coupling or oxygen consumption. The antimycobacterial compound is bactericidal and potent against Mtb in macrophages without inducing phenotypic changes in biofilm formation, planktonic bacteria, or being toxic to zebrafish larvae. Combining GaMF1.39 with the NADH dehydrogenase inhibitor clofazimine, the cyt- bcc:aa 3 inhibitor Telacebec, or the F-ATP synthase inhibitor TBAJ-876 showed enhanced whole ATP synthesis inhibition and anti-tuberculosis activity. These results suggest that GaMF1.39 may add value to a compound combination targeting oxidative phosphorylation for tuberculosis treatment. IMPORTANCE New drugs are needed to combat multidrug-resistant tuberculosis. The electron transport chain (ETC) maintains the electrochemical potential across the cytoplasmic membrane and allows the production of ATP, the energy currency of any living cell. The mycobacterial engine F-ATP synthase catalyzes the formation of ATP and has come into focus as an attractive and rich drug target. Recent deep insights into these mycobacterial F 1 F O -ATP synthase elements opened the door for a renaissance of structure-based target identification and inhibitor design. In this study, we present the GaMF1.39 antimycobacterial compound, targeting the rotary subunit γ of the biological engine. The compound is bactericidal, inhibits infection ex vivo , and displays enhanced anti-tuberculosis activity in combination with ETC inhibitors, which promises new strategies to shorten tuberculosis chemotherapy.

Funder

National Research Foundation Singapore

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Cell Biology,Microbiology (medical),Genetics,General Immunology and Microbiology,Ecology,Physiology

Link

https://journals.asm.org/doi/pdf/10.1128/spectrum.02282-23

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