A Modified BPaL Regimen for Tuberculosis Treatment replaces Linezolid with Inhaled Spectinamides

Author:

Ali Malik Zohaib123,Dutt Taru S12,MacNeill Amy2,Walz Amanda12,Pearce Camron123,Lam Ha12,Philp Jamie12,Patterson Johnathan12,Henao-Tamayo Marcela12,Lee Richard E4,Liu Jiuyu4,Robertson Gregory T12ORCID,Hickey Anthony J5,Meibohm Bernd6ORCID,Gonzalez-Juarrero Mercedes12ORCID

Affiliation:

1. Mycobacteria Research Laboratories, Colorado State University

2. Microbiology, Immunology and Pathology, Colorado State University

3. Program in Cell & Molecular Biology, Colorado State University

4. Department of Chemical Biology and Therapeutics, St. Jude Children’s Research Hospital

5. Technology Advancement and Commercialization

6. Department of Pharmaceutical Sciences, Univeof Tennessee Health Science Center

Abstract

The Nix-TB clinical trial evaluated a new 6-month regimen containing three-oral- drugs; bedaquiline (B), pretomanid (Pa) and linezolid (L) (BPaL regimen) for treatment of tuberculosis (TB). This regimen achieved remarkable results as almost 90% of the multidrug resistant (MDR) or extensively drug resistant (XDR) TB participants were cured but many patients also developed severe adverse events (AEs). The AEs were associated with the long-term administration of the protein synthesis inhibitor linezolid. Spectinamide 1599 is also a protein synthesis inhibitor of Mycobacterium tuberculosis with an excellent safety profile but which lacks oral bioavailability. Here, we propose to replace L in the BPaL regimen with spectinamide (S) administered via inhalation and we demonstrate that inhaled spectinamide 1599, combined with BPa ––BPaS regimen––has similar efficacy to that of BPaL regimen while simultaneously avoiding the L-associated AEs. The BPaL and BPaS regimens were compared in the BALB/c and C3HeB/FeJ murine chronic TB efficacy models. After 4-weeks of treatment, both regimens promoted equivalent bactericidal effect in both TB murine models. However, treatment with BPaL resulted in significant weight loss and the complete blood count suggested development of anemia. These effects were not similarly observed in mice treated with BPaS. BPaL and BPa, but no the BPaS treatment, also decreased myeloid to erythroid ratio suggesting the S in the BPaS regimen was able to recover this effect. Moreover, the BPaL also increased concentration of proinflammatory cytokines in bone marrow compared to mice receiving BPaS regimen. During therapy both regimens improved the lung lesion burden, reduced neutrophil and cytotoxic T cells counts while increased the number of B and helper and regulatory T cells. These combined data suggest that inhaled spectinamide 1599 combined with BPa is an effective TB regimen that avoids L-associated AEs.

Publisher

eLife Sciences Publications, Ltd

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