AI Article Synopsis
- * The study focuses on how two Mycobacterium tuberculosis strains respond to delamanid, a recently approved drug, revealing that its action is similar to another drug, pretomanid, in the same drug class.
- * While delamanid inhibits cell wall synthesis, the study found that its most significant impact is on aerobic respiration, indicating that respiratory poisoning is key to its effectiveness, especially noting the role of poorly understood genes in its action.
Article Abstract
Tuberculosis (TB) is the most deadly infectious disease worldwide. To reduce TB incidence and counter the spread of multidrug resistant TB, the discovery and characterization of new drugs is essential. In this study, the transcriptional response of two Mycobacterium tuberculosis strains to a pressure of the recently approved delamanid is investigated. Total RNA sequencing revealed that the response to this bicyclic nitroimidazole shows many similarities with pretomanid, an anti-tuberculous drug from the same class. Although delamanid is found to inhibit cell wall synthesis, the expression of genes involved in this process were only mildly affected. In contrast, a clear parallel was found with components that affect aerobic respiration. This demonstrates that, besides the inhibition of cell wall synthesis, respiratory poisoning plays a fundamental role in the bactericidal effect of delamanid. Remarkably, the most highly induced genes comprise poorly characterized genes for which functional characterization might hint to the target molecule(s) of delamanid and its exact mode(s) of action.
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| http://dx.doi.org/10.1016/j.tube.2019.05.002 | DOI Listing |
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