Levofloxacin Pharmacokinetics/Pharmacodynamics, Dosing, Susceptibility Breakpoints, and Artificial Intelligence in the Treatment of Multidrug-resistant Tuberculosis

Deshpande, Devyani; Pasipanodya, Jotam G.; Mpagama, Stellah; Bendet, Paula; Srivastava, Shashikant; Koeuth, Thearith; Lee, Pooi S; Bhavnani, Sujata M.; Ambrose, Paul G.; Thwaites, Guy; Heysell, Scott K; Gumbo, Tawanda

doi:10.1093/cid/ciy611

Cited by 76 publications

(90 citation statements)

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“…First, we did not examine d-cycloserine in combination with other drugs for synergistic effects, which could potentially lower the exposures of d-cycloserine needed. Second, in contrast to our work with gatifloxacin, levofloxacin, and ethionamide, we had no clinical data to validate the doses or susceptibility breakpoints we identified [18,51,55]. Third, we relied on the Sensititre assay, which is not endorsed by WHO and could differ from conventional media, to define a tentative ECOFF.…”

Section: Discussionmentioning

confidence: 92%

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d-Cycloserine Pharmacokinetics/Pharmacodynamics, Susceptibility, and Dosing Implications in Multidrug-resistant Tuberculosis: A Faustian Deal

Deshpande

Alffenaar

Köser

et al. 2018

Clinical Infectious Diseases

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Background. d-cycloserine is used to treat multidrug-resistant tuberculosis. Its efficacy, contribution in combination therapy, and best clinical dose are unclear, also data on the d-cycloserine minimum inhibitory concentration (MIC) distributions is scant. Methods. We performed a systematic search to identify pharmacokinetic and pharmacodynamic studies performed with d-cycloserine. We then performed a combined exposure-effect and dose fractionation study of d-cycloserine in the hollow fiber system model of tuberculosis (HFS-TB). In parallel, we identified d-cycloserine MICs in 415 clinical Mycobacterium tuberculosis (Mtb) isolates from patients. We utilized these results, including intracavitary concentrations, to identify the clinical dose that would be able to achieve or exceed target exposures in 10 000 patients using Monte Carlo experiments (MCEs). Results. There were no published d-cycloserine pharmacokinetics/pharmacodynamics studies identified. Therefore, we performed new HFS-TB experiments. Cyloserine killed 6.3 log 10 colony-forming units (CFU)/mL extracellular bacilli over 28 days. Efficacy was driven by the percentage of time concentration persisted above MIC (%T MIC), with 1.0 log 10 CFU/mL kill achieved by %T MIC = 30% (target exposure). The tentative epidemiological cutoff value with the Sensititre MYCOTB assay was 64 mg/L. In MCEs, 750 mg twice daily achieved target exposure in lung cavities of 92% of patients whereas 500 mg twice daily achieved target exposure in 85% of patients with meningitis. The proposed MCE-derived clinical susceptibility breakpoint at the proposed doses was 64 mg/L. Conclusions. Cycloserine is cidal against Mtb. The susceptibility breakpoint is 64 mg/L. However, the doses likely to achieve the cidality in patients are high, and could be neurotoxic.

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Section: Discussionmentioning

confidence: 92%

“…Second, d-cycloserine had impressive kill rates against Mtb in the HFS-TB, which rivaled some of the first-line compounds and fluoroquinolones [18,36,51]. Thus the drug is not "static, " as has been traditionally thought.…”

Section: Discussionmentioning

confidence: 97%

d-Cycloserine Pharmacokinetics/Pharmacodynamics, Susceptibility, and Dosing Implications in Multidrug-resistant Tuberculosis: A Faustian Deal

Deshpande

Alffenaar

Köser

et al. 2018

Clinical Infectious Diseases

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“…Furthermore, a trend toward moderately positive correlation (r s ϭ 0.379; P ϭ 0.021) was observed when Lfx C min in saliva was evaluated to predict its AUC 0 -24 in plasma (r ϭ 0.38; estimated linear regression equation). When the saliva C min was Ͻ2 mg/liter, a proportion of patients had a plasma AUC 0 -24 below the desired level, 146, given the MIC was 1 mg/liter (12).…”

Section: Resultsmentioning

confidence: 99%

“…Therefore, measuring Lfx concentrations in plasma or other alternative matrices (saliva and dried blood spots) could help clinicians make informed dosing decisions, especially now, as the TB treatment marches toward individualization, therapeutic drug monitoring (TDM) using saliva sampling might become a game changer in TB treatment due to specific advantages over plasma sampling, in low-resource settings (10,11). The efficacy of Lfx is predicted by AUC 0 -24 and MIC (12). Given as a monotherapy, the hollow-fiber infection model on TB recently established a Lfx target of 146 for maximum bacterial kill (80% effective concentration) and 360 for the prevention of acquired drug resistance (12).…”

mentioning

confidence: 99%

“…The efficacy of Lfx is predicted by AUC 0 -24 and MIC (12). Given as a monotherapy, the hollow-fiber infection model on TB recently established a Lfx target of 146 for maximum bacterial kill (80% effective concentration) and 360 for the prevention of acquired drug resistance (12). Therefore, a plasma AUC 0 -24 above 75 (if the MIC is 0.5 mg/liter) or 146 (if the MIC is 1 mg/liter) will be needed to attain the optimal target exposure for efficacy.…”

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confidence: 99%

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Evaluation of Saliva as a Potential Alternative Sampling Matrix for Therapeutic Drug Monitoring of Levofloxacin in Patients with Multidrug-Resistant Tuberculosis

Ghimire

Maharjan

Jongedijk

et al. 2019

Antimicrob Agents Chemother

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Saliva may be a useful alternative matrix for monitoring levofloxacin concentrations in multidrug-resistant tuberculosis (MDR-TB) patients. The objectives of this study were (i) to evaluate the correlation between plasma and salivary levofloxacin (Lfx) concentrations in MDR-TB patients and (ii) to gauge the possibility of using saliva as an alternative sampling matrix for therapeutic drug monitoring of Lfx in areas where TB is endemic. This was a prospective pharmacokinetic study that enrolled MDR-TB patients receiving levofloxacin (750-to 1,000-mg once-daily dosing) under standardized treatment regimen in Nepal. Paired blood and saliva samples were collected at steady state. Lfx concentrations were quantified using liquid chromatography-tandem mass spectrometry. Pharmacokinetic parameters were calculated using noncompartmental kinetics. Lfx drug exposures were evaluated in 23 MDR-TB patients. During the first month, the median (interquartile range [IQR]) areas under the concentration-time curve from 0 to 24 h (AUC 0 -24 ) were 67.09 (53.93 to 98.37) mg · h/liter in saliva and 99.91 (76.80 to 129.70) mg · h/liter in plasma, and the saliva plasma (S/P) ratio was 0.69 (0.53 to 0.99). Similarly, during the second month, the median (IQR) AUC 0 -24 were 75.63 (61.45 to 125.5) mg · h/liter in saliva and 102.7 (84.46 to 131.9) mg · h/liter in plasma, with an S/P ratio of 0.73 (0.66 to 1.18). Furthermore, large inter-and intraindividual variabilities in Lfx concentrations were observed. This study could not demonstrate a strong correlation between plasma and saliva Lfx levels. Despite a good Lfx penetration in saliva, the variability in individual saliva-to-plasma ratios limits the use of saliva as a valid substitute for plasma. Nevertheless, saliva could be useful in semiquantitatively predicting Lfx plasma levels. (This study has been registered at ClinicalTrials.gov under identifier NCT03000517.)

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Optimal therapy design with tumor microenvironment normalization

Stuber

2022

AIChE Journal

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Tumor microenvironment (TME) normalization improves efficacy by increasing anticancer nanocarrier delivery by restoring transvascular pressure gradients that induce convection. However, transport depends on TME biophysics, normalization dose, and nanocarrier size. With increased understanding, we could use computation to personalize normalization amount and nanocarrier size. Here, we use deterministic global dynamic optimization with novel bounding routines to validate mechanistic models against in vivo data. We find that normalization with dexamethasone increases the maximum transvascular convection rate of nanocarriers by 48‐fold, the tumor volume fraction with convection by 61%, and the total amount of convection by 360%. Nonetheless, 22% of the tumor still lacks convection. These findings underscore both the effectiveness and limits of normalization. Using artificial neural network surrogate modeling, we demonstrate the feasibility of rapidly determining the dexamethasone dose and nanocarrier size to maximize accumulation. Thus, this digital testbed quantifies transport and performs therapy design.

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Levofloxacin Pharmacokinetics/Pharmacodynamics, Dosing, Susceptibility Breakpoints, and Artificial Intelligence in the Treatment of Multidrug-resistant Tuberculosis

Cited by 76 publications

References 50 publications

d-Cycloserine Pharmacokinetics/Pharmacodynamics, Susceptibility, and Dosing Implications in Multidrug-resistant Tuberculosis: A Faustian Deal

d-Cycloserine Pharmacokinetics/Pharmacodynamics, Susceptibility, and Dosing Implications in Multidrug-resistant Tuberculosis: A Faustian Deal

Evaluation of Saliva as a Potential Alternative Sampling Matrix for Therapeutic Drug Monitoring of Levofloxacin in Patients with Multidrug-Resistant Tuberculosis

Optimal therapy design with tumor microenvironment normalization

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