Emergence of resistance to the antiparasitic selamectin inMycobacterium smegmatisis improbable and contingent on cell wall integrity

Abstract

AbstractTuberculosis remains the deadliest infectious disease of the 21stcentury. New antimicrobials are needed to improve treatment outcomes and enable therapy shortening. Drug repurposing is an alternative to the traditional drug discovery process. The avermectins are a family of macrocyclic lactones with anthelmintic activity active againstMycobacterium tuberculosis. However, their mode of action in mycobacteria remains unknown.In this study, we employed traditional mutant isolation approaches usingMycobacterium smegmatis, a non-pathogenicMycobacterium tuberculosissurrogate. We were only able to isolate mutants with decreased susceptibility to selamectin using the ΔnucSmutatorM. smegmatisstrain. This phenotype was caused by mutations inmps1andmmpL11. Two of these mutants were used for a second experiment in which high-level selamectin-resistant mutants were isolated; however, specific mutations driving the phenotypic change to high-level resistance could not be identified. The susceptibility to selamectin in these mutants was restored to the basal level by subinhibitory concentrations of ethambutol. The selection of ethambutol resistance in a high-level selamectin-resistant mutant also resulted in multiple colonies becoming susceptible to selamectin again. These colonies carried mutations inembB, suggesting that integrity of the cell envelope is a prerequisite for selamectin resistance. The absence of increased susceptibility to selamectin in anembBdeletion strain demonstrated that the target of selamectin is not cytosolic. Our data show that concurrence of specific multiple mutations and complete integrity of the mycobacterial envelope are necessary for selamectin resistance. Our studies provide first-time insights into the antimycobacterial mode of action of the antiparasitic avermectins.