The therapeutic repertoire for tuberculosis (TB) remains limited despite the existence of many TB drugs that are highly active in models and possess clinical utility. Underlying the lack of efficacy is the inability of TB drugs to penetrate microenvironments inhabited by the causative agent, Mycobacterium tuberculosis, including host alveolar macrophages. Here, we determined the ability of the phenoxazine PhX1 previously shown to be active against M.
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