Abstract
BackgroundDirectly observed therapy (DOT) is a widely recommended and promoted strategy to manage tuberculosis (TB), however, there is still disagreement about the role of DOT in TB control and the impact it has on reducing the acquisition and transmission of drug resistant TB. This study compares the portion of drug resistant genotype clusters, representing recent transmission, within and between communities implementing programs differing only in their directly observed therapy (DOT) practices.MethodsGenotype clusters were defined as 2 or more patient members with matching IS6110 restriction fragment length polymorphism (RFLP) and spoligotype patterns from all culture-positive tuberculosis cases diagnosed between January 1, 1995 and December 31, 2001. Logistic regression was used to compute maximum-likelihood estimates of odds ratios (ORs) and 95% confidence intervals (CIs) comparing cluster members with and without drug resistant isolates. In the universal DOT county, all patients received doses under direct observation of health department staff; whereas in selective DOT county, the majority of received patients doses under direct observation of health department staff, while some were able to self-administer doses.ResultsIsolates from 1,706 persons collected during 1,721 episodes of tuberculosis were genotyped. Cluster members from the selective DOT county were more than twice as likely than cluster members from the universal DOT county to have at least one isolate resistant to isoniazid, rifampin, and/or ethambutol (OR = 2.3, 95% CI: 1.7, 3.1). Selective DOT county isolates were nearly 5 times more likely than universal DOT county isolates to belong to clusters with at least 2 resistant isolates having identical resistance patterns (OR = 4.7, 95% CI: 2.9, 7.6).ConclusionsUniversal DOT for tuberculosis is associated with a decrease in the acquisition and transmission of resistant tuberculosis.
Highlights
Observed therapy (DOT) is a widely recommended and promoted strategy to manage tuberculosis (TB), there is still disagreement about the role of directly observed therapy (DOT) in TB control and the impact it has on reducing the acquisition and transmission of drug resistant TB
Persons excluded from analysis because there was no viable clinical isolate of M. tuberculosis did not differ statistically from those with viable isolates by age (P = 0.44), gender (P = 0.56), or race (P = 0.70)
HIV status was not an effect modifier. This is the first study to combine molecular genotyping techniques and drug susceptibilities to demonstrate that DOT for tuberculosis is associated with less initial drug resistance and less transmission of drug resistant organisms
Summary
Observed therapy (DOT) is a widely recommended and promoted strategy to manage tuberculosis (TB), there is still disagreement about the role of DOT in TB control and the impact it has on reducing the acquisition and transmission of drug resistant TB. This study compares the portion of drug resistant genotype clusters, representing recent transmission, within and between communities implementing programs differing only in their directly observed therapy (DOT) practices. Worldwide tuberculosis transmission continues despite intensive control efforts and availability of highly effective, relatively inexpensive treatment regimens [1,2,3]. The time commitment for successful treatment of tuberculosis is longer than required for most acute medical conditions [4,5]. Additional tuberculosis transmission and the development of drug resistance can result when tuberculosis treatment fails due to noncompliance [6].
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