Abstract:Collateral sensitivity (CS)-based antibiotic treatments, where increased antibiotic resistance to one antibiotic leads to increased antibiotic sensitivity of second antibiotic, could constitute a strategy to limit emergence of antibiotic resistance. However, it is unclear how to design CS-based dosing schedules that effectively suppress resistance. Here, we use a mathematical modelling approach incorporating pharmacokinetic and pharmacodynamic features to simulate bacterial population dynamics for different co… Show more
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