RecruitingNCT05824988

Drug Exposure and Minimum Inhibitory Concentration in the Treatment of MAC Lung Disease

Drug Exposure and Minimum Inhibitory Concentration in the Treatment of Mycobacterium Avium Complex Lung Disease: a Prospective Observational Cohort Study

Sponsor

Shanghai Pulmonary Hospital, Shanghai, China

Enrollment

100 participants

Start Date

Apr 14, 2023

Study Type

OBSERVATIONAL

Conditions

Mycobacterium Infections Gram-Positive Bacterial Infections Mycobacterium Avium Complex Mycobacterium Avium-Intracellulare Infection

Summary

The incidence and prevalence of nontuberculous mycobacteria (NTM) infections have gradually increased over the years worldwide (1-3). In China, Mycobacterium avium complex (MAC) was the most prevalent NTM specie (4), while challenged by long treatment duration, frequent drug-induced adverse events, lack of treatment alternatives, poor treatment outcome and high recurrence rate (5, 6). In order to maximize the efficacy of the few available drugs and prevent the development of drug resistance, ensuring adequate plasma drug concentrations are of importance. Despite the role of pathogen susceptibility, determined by minimum inhibitory concentration (MIC), is non-negligible, the evidences regarding its association with treatment outcome are limited, especially for rifamycin and ethambutol. The difficulties in explaining the clinical values of MIC might partially be attributed to the lack of in vivo drug exposure data, which cannot be accurately predicted by the dose administered because of between-patient pharmacokinetic variability (7). Therapeutic drug monitoring (TDM) is a strategy to guide and personalize treatment by measuring plasma drug concentrations and pathogen susceptibility, which might have the potential to improve treatment response to MAC lung disease. In this observational study, the hypothesis is that the drug exposure and/or MIC of antimycobacterial drugs are correlated to the treatment response of MAC lung disease, which is assessed from the perspective of treatment outcome, mycobacterial culture negative conversion, lung function, radiological presentation and self-reported quality of life. Consenting adult patients with culture-positive MAC lung disease will be recruited in study hospital. Respiratory samples (sputum and/or bronchoalveolar lavage fluid) will be collected regularly for mycobacterial culture on the basis of BACTEC MGIT 960 system and MIC will be determined using a commercial broth microdilution plate. Drug concentrations will be measured at 1 and/or 6 months after treatment initiation using liquid chromatography tandem mass spectrometry (LC-MS/MS). The final treatment outcome is recorded at the end of MAC treatment and defined according to an NTM-NET consensus statement (8).

Eligibility

Min Age: 18 Years

Plain Language Summary

Simplified for easier understanding

This study is investigating how drug concentrations in the blood relate to treatment outcomes in patients being treated for Mycobacterium avium complex (MAC) lung disease. MAC is a type of non-tuberculosis mycobacterial infection that primarily affects the lungs, particularly in older adults and people with underlying lung conditions. Treatment requires long courses of multiple antibiotics, and outcomes vary significantly between patients — possibly because drug levels in the blood differ from person to person. Adults aged 18 and older who have confirmed MAC lung disease, are being treated at Shanghai Pulmonary Hospital with a standard regimen including macrolides, rifamycin, and ethambutol, and have provided written consent are eligible. Pregnant patients, those with mixed mycobacterial infections (including TB), patients who have been on antimycobacterial treatment for more than one month, and ICU patients are not eligible. Participants will have blood samples taken during treatment to measure drug levels. These will be correlated with minimum inhibitory concentrations (MICs) — the lowest drug concentration that stops bacterial growth — and clinical outcomes. This is an observational study requiring no change to standard care. The research matters because optimizing drug dosing based on individual blood levels could significantly improve cure rates in a disease where treatment failure and relapse are frustratingly common.

This summary was AI-generated to explain the trial in plain language. It is not medical advice. Always discuss eligibility with your doctor before enrolling in a clinical trial.

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Interventions

OTHERDrug exposure

Drug concentrations will be measured after one-month antimycobacterial treatment. Area under drug concentration-time curve (AUC) and maximum concentration (Cmax) will be calculated.