Contribution of pretomanid to novel regimens containing bedaquiline with either linezolid or moxifloxacin and pyrazinamide in murine models of tuberculosis

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

doi:10.1101/514661

Cited by 7 publications

(12 citation statements)

References 31 publications

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“…Importantly, we did not observe selection of higher level, or "second-step" BDQ resistance despite treating the Rv0678 mutant infection with BDQ or TBAJ-587 alone. This is likely a function of the low frequency of viable spontaneous atpE mutants and their fitness costs observed in vivo (27). were formulated in 20% hydroxypropyl-β-cyclodextrin solution acidified with 1.5% 1N HCl.…”

Section: Discussionmentioning

confidence: 99%

“…At D0, the mean frequencies of CFU able to grow on agar containing 0.06 and 0.25 µg/ml of BDQ were 4.2x10 -5 and 1.8x10 -5 , respectively. Plates containing BDQ 0.06 µg/ml were used to quantify the resistant subpopulation at subsequent time points, based on prior evidence of its effectiveness for quantifying mutants with low-level resistance to BDQ (27). All mice infected with M. tuberculosis H37Rv and treated with BDQ monotherapy at 25 mg/kg for one or two months demonstrated selective amplification of BDQ-resistant CFU, which represented approximately 3% and 18% of the recovered CFU after one and two months, respectively (Table 1).…”

Section: Selection Of Drug-resistant Mutants (I) Mice Infected With mentioning

confidence: 99%

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Comparative Efficacy of the Novel Diarylquinoline TBAJ-587 and Bedaquiline against a Resistant Rv0678 Mutant in a Mouse Model of Tuberculosis

Converse

Upton

et al. 2021

Antimicrob Agents Chemother

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Since its conditional approval in 2012, bedaquiline (BDQ) has been a valuable tool for treatment of drug-resistant tuberculosis. More recently, a novel short-course regimen combining BDQ with pretomanid and linezolid won approval to treat highly drug-resistant tuberculosis. Clinical reports of emerging BDQ resistance have identified mutations in Rv0678 that de-repress the expression of the MmpL5/MmpS5 efflux transporter as the most common cause. Because the effect of these mutations on bacterial susceptibility to BDQ is relatively small (e.g., 2-8x MIC shift), increasing the BDQ dose would increase antibacterial activity but also pose potential safety concerns, including QTc prolongation. Substitution of BDQ with another diarylquinoline with superior potency and/or safety has the potential to overcome these limitations. TBAJ-587 has greater in vitro potency than BDQ, including against Rv0678 mutants, and may offer a larger safety margin. Using a mouse model of tuberculosis and different doses of BDQ and TBAJ-587, we found that against wild-type M. tuberculosis H37Rv and an isogenic Rv0678 mutant, TBAJ-587 has greater efficacy against both strains than BDQ, whether alone or in combination with pretomanid and either linezolid or moxifloxacin and pyrazinamide. TBAJ-587 also reduced the emergence of resistance to diarylquinolines and pretomanid.

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Section: Discussionmentioning

confidence: 99%

Section: Selection Of Drug-resistant Mutants (I) Mice Infected With mentioning

confidence: 99%

Comparative Efficacy of the Novel Diarylquinoline TBAJ-587 and Bedaquiline against a Resistant Rv0678 Mutant in a Mouse Model of Tuberculosis

Converse

Upton

et al. 2021

Antimicrob Agents Chemother

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show abstract

“…Importantly, we did not observe selection of higher level, or “second-step” BDQ resistance despite treating the Rv0678 mutant infection with BDQ or TBAJ-587 alone. This is likely a function of the low frequency of viable spontaneous atpE mutants and their fitness costs observed in vivo (31). Although atpE mutations have been identified in a small number of BDQ-resistant clinical isolates to date (32, 33), Rv0678 mutations have been more prevalent.…”

Section: Discussionmentioning

confidence: 99%

“…The laboratory strain, M. tuberculosis H37Rv, and a spontaneous bedaquiline-resistant mutant with an IS 6110 insertion in Rv0678 at aa116/nt349 were used in this study. The Rv0678 mutant was previously identified as BDQ-8 when it was isolated from an untreated mouse infected by H37Rv (31). The Rv0678 mutation and the absence of other mutations in genes associated with drug resistance were confirmed by whole genome sequencing.…”

Section: Methodsmentioning

confidence: 99%

Comparative efficacy of the novel diarylquinoline TBAJ-587 and bedaquiline against a resistantRv0678mutant in a mouse model of tuberculosis

Converse

Upton

et al. 2020

Preprint

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Since its conditional approval in 2012, bedaquiline (BDQ) has been a valuable tool for treatment of drug-resistant tuberculosis. More recently, a novel short-course regimen combining BDQ with pretomanid and linezolid won approval to treat highly drug-resistant tuberculosis. Clinical reports of emerging BDQ resistance have identified mutations in Rv0678 that de-repress the expression of the MmpL5/MmpS5 efflux transporter as the most common cause. Because the effect of these mutations on bacterial susceptibility to BDQ is relatively small (e.g., 2-8× MIC shift), increasing the BDQ dose would increase antibacterial activity but also pose potential safety concerns, including QTc prolongation. Substitution of BDQ with another diarylquinoline with superior potency and/or safety has the potential to overcome these limitations. TBAJ-587 has greater in vitro potency than BDQ, including against Rv0678 mutants, and may offer a larger safety margin. Using a mouse model of tuberculosis and different doses of BDQ and TBAJ-587, we found that against wild-type M. tuberculosis H37Rv and an isogenic Rv0678 mutant, TBAJ-587 has greater efficacy against both strains than BDQ, whether alone or in combination with pretomanid and either linezolid or moxifloxacin and pyrazinamide. TBAJ-587 also reduced the emergence of resistance to diarylquinolines and pretomanid.

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“…Finally, the addition of PMD to BZ does not yield an improvement in EBA 7–14 (from 0.152 to 0.146) 49 . Overall, these results indicate that whilst the use of PMD as companion drug may contribute to a lower relapse rate, 50 it does not appear to improve the overall antimicrobial activity of the combination.…”

Section: Discussionmentioning

confidence: 83%

Evaluation of pharmacokinetic‐pharmacodynamic relationships and selection of drug combinations for tuberculosis

Muliaditan

Pasqua

2020

Brit J Clinical Pharma

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Despite evidence of the efficacy of anti-tubercular drug regimens in clinical practice, the rationale underpinning the selection of doses and companion drugs for combination therapy remains empirical. Novel methods are needed to optimise the antibacterial activity in combination therapies. A drug-disease modelling framework for rational selection of dose and drug combinations in tuberculosis is presented here. Methods: A model-based meta-analysis was performed to assess the antibacterial activity of different combinations in infected mice. Data retrieved from the published literature were analysed using a two-state bacterial growth dynamics model, including fast-and slow-growing bacterial populations. The contribution of each drug to the overall antibacterial activity of the combination was parameterised as relative change to the potency of the backbone drug (EC 50-F and/or EC 50-S). Rifampicin and bedaquiline were selected as paradigm drugs to evaluate the predictive performance of the modelling approach. Results: Pyrazinamide increased the potency (EC 50-F and EC 50-S) of rifampicin (RZ) and bedaquiline (BZ) by almost twofold. By contrast, pretomanid and isoniazid were found to worsen the antibacterial activity of BZ and RZ, respectively. Following extrapolation of in vivo pharmacokinetic-pharmacodynamic relationships, the dose of rifampicin showing maximum bactericidal effect in tuberculosis patients was predicted to be 70 mgÁkg −1 when given in combination with pyrazinamide. Conclusions: The use of a drug-disease modelling framework may provide a more robust rationale for extrapolation and selection of dose and companion drugs in humans. Our analysis demonstrates that RZ and BZ should be considered as a backbone therapy in prospective novel combination regimens against tuberculosis.

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Contribution of pretomanid to novel regimens containing bedaquiline with either linezolid or moxifloxacin and pyrazinamide in murine models of tuberculosis

Cited by 7 publications

References 31 publications

Comparative Efficacy of the Novel Diarylquinoline TBAJ-587 and Bedaquiline against a Resistant Rv0678 Mutant in a Mouse Model of Tuberculosis

Comparative Efficacy of the Novel Diarylquinoline TBAJ-587 and Bedaquiline against a Resistant Rv0678 Mutant in a Mouse Model of Tuberculosis

Comparative efficacy of the novel diarylquinoline TBAJ-587 and bedaquiline against a resistantRv0678mutant in a mouse model of tuberculosis

Evaluation of pharmacokinetic‐pharmacodynamic relationships and selection of drug combinations for tuberculosis

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