Repurposing AZD-5991 for inhibiting growth and biofilm formation ofStaphylococcus aureusby disrupting the cell membrane and targeting FabI

Staphylococcus aureusinfections have already become a major threat to public health worldwide. Drug resistance and biofilm formation are two critical factors that significantly affect the efficacy of the antimicrobial treatment ofS. aureusinfections using conventional antibiotics. Therefore, the discovery of novel antimicrobial agents with potent antibacterial and antibiofilm activity has become a hotspot in recent years. Here, we first demonstrated the remarkable inhibitory activity of AZD-5991, a selective Mcl-1 inhibitor, againstS. aureus. The MIC₅₀and MIC₉₀of AZD-5991 againstS. aureuswere 12.5 μM, and AZD-5991 significantly inhibited the growth ofS. aureusat a subinhibitory concentration of 1/2 × MIC. Besides, AZD-5991 displayed bactericidal activity and a robust capacity for inhibiting biofilm formation againstS. aureuswith very low drug toxicity against host cell lines. Our data demonstrated the disruption ofS.aureuscell integrity by AZD-5991 through membrane permeability assays and the ingredients of the bacterial phospholipids could neutralize the antibacterial activity of AZD-5991. Moreover, whole-genome sequencing and proteomic analysis were also applied to gain insights into the possible impact of AZD-5991 on the fatty metabolism ofS. aureus. Furthermore, the antibacterial activity of AZD-5991 was significantly elevated by exogenous fatty acids linoleic acid (C18:2 Δ 9,12) and arachidonic acid (C20:4 Δ 5,8,11,14). Lastly, the biolayer interferometry assay supported the direct interaction of AZD-5991 with FabI, a necessary protein related closely to bacterial growth and fatty acid metabolism. Conclusively, this study suggests that AZD-5991 could inhibit the planktonic growth and biofilm formation ofS. aureusby disrupting the cell membrane and targeting FabI. AZD-5991 might be a promising new antibiotic candidate for the antimicrobial treatment ofS. aureusinfections resistant to traditional clinical drugs.