Tuberculosis remains a major infectious cause of morbidity and mortality worldwide. Current antibiotic regimens, constructed prior to the development of modern pharmacokinetic-pharmacodynamic (PK-PD) tools, are based on incomplete understanding of exposure-response relationships in drug susceptible and multidrug resistant tuberculosis. Preclinical and population PK data suggest that clinical PK-PD studies may enable therapeutic drug monitoring for some agents and revised dosing for others. Future clinical PK-PD challenges include: incorporation of PK methods to assay free concentrations for all active metabolites; selection of appropriate early outcome measures which reflect therapeutic response; elucidation of genetic contributors to interindividual PK variability; conduct of targeted studies on special populations (including children); and measurement of PK-PD parameters at the site of disease.
Keyphrases
- multidrug resistant
- mycobacterium tuberculosis
- pulmonary tuberculosis
- hiv aids
- case control
- emergency department
- young adults
- stem cells
- gene expression
- adverse drug
- high throughput
- escherichia coli
- type diabetes
- ms ms
- pseudomonas aeruginosa
- drug delivery
- machine learning
- acinetobacter baumannii
- skeletal muscle
- big data
- weight loss
- current status
- human immunodeficiency virus
- antiretroviral therapy