Abstract
Tuberculosis (TB) is considered as one of the most serious threats to public health in many parts of the world. The threat is even more severe in the developing countries where there is a lack of advanced medical amenities and contemporary anti-TB drugs. In such situations, dosage optimization of existing medication regimens seems to be the only viable option. Therapeutic drug monitoring study results suggest that high-dose treatment regimens can compensate the low serum concentration of anti-TB drugs and shorten the therapy duration. The article presents a critical review on the possible changes that occur in the host and the pathogen upon the administration of standard and high-dose regimens. Some of the most common factors that are responsible for low anti-TB drug concentrations in the serum are differences in hosts’ body weight, metabolic processing of the drug, malabsorption and/or drug–drug interaction. Furthermore, failure to reach the cavitary pulmonary and extrapulmonary tissues also contributes to the therapeutic inefficiency of the drugs. In such conditions, administration of higher doses can help in compensating the pathogenic outcomes of enhancement of the pathogen’s physical barriers, efflux pumps and genetic mutations. The present article also presents a summary of the recorded treatment outcomes of clinical trials that were conducted to test the efficacy of administration of high dose of anti-tuberculosis drugs. This review will help physicians across the globe to understand the underlying pathophysiological changes (including side effects) that dictate the clinical outcomes in patients administered with standard and/or high dose anti-TB drugs.
Highlights
Tuberculosis is a highly contagious disease caused due to Mycobacterium tuberculosis infection
These results indicate that the metabolic state of M. tuberculosis bacteria significantly affect its susceptibility to antimicrobials, and exert a profound effect on the optimization of anti-TB drug dosages required to maximize the reduction in M. tuberculosis load and minimize the emergence of drug resistance
The results showed that the high dose of 35 mg/ kg RIF was safe and it could help in reducing the time of culture conversion in liquid media; and can be considered as a promising component of future, shorter treatment regimens [96]
Summary
Tuberculosis is a highly contagious disease caused due to Mycobacterium tuberculosis infection. The study conducted by de Steenwinkel et al investigated the time-kill kinetics of anti-TB drugs in relation to the metabolic activity of M. tuberculosis and found that when compared with highly active mycobacteria elimination of the susceptible lowactivity mycobacteria requires 64-fold increase in INH concentration and a fourfold increase in RIF concentration, whereas amikacin (AMK) was effective irrespective of the mycobacteria’s metabolic state [63].
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