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Pharmacodynamic considerations of collateral sensitivity in design of antibiotic treatment regimen

机译:抗生素治疗方案设计中附带敏感性的药效学考虑

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IntroductionAntibiotics have greatly reduced the morbidity and mortality due to infectious diseases. Although antibiotic resistance is not a new problem, its breadth now constitutes a significant threat to human health. One strategy to help combat resistance is to find novel ways to use existing drugs, even those that display high rates of resistance. For the pathogens Escherichia coli and Pseudomonas aeruginosa, pairs of antibiotics have been identified for which evolution of resistance to drug A increases sensitivity to drug B and vice versa. These research groups have proposed cycling such pairs to treat infections, and similar treatment strategies are being investigated for various cancer forms as well. While an exciting treatment prospect, no cycling experiments have yet been performed with consideration of pharmacokinetics and pharmacodynamics. To test the plausibility of such schemes and optimize them, we create a mathematical model with explicit pharmacokinetic/pharmacodynamic considerations.
机译:简介抗生素已大大降低了由于传染病引起的发病率和死亡率。尽管抗生素耐药性不是一个新问题,但其广度现在对人类健康构成了重大威胁。帮助抗药性的一种策略是找到使用现有药物的新颖方法,即使那些药物显示出高抗药性。对于病原体大肠杆菌和铜绿假单胞菌,已鉴定出成对的抗生素,其对药物A的抗性演变会增加对药物B的敏感性,反之亦然。这些研究小组已提议循环使用这种配对来治疗感染,并且正在针对各种癌症形式研究类似的治疗策略。尽管有令人兴奋的治疗前景,但尚未进行考虑药代动力学和药效学的循环实验。为了测试此类方案的合理性并对其进行优化,我们创建了具有明确药代动力学/药效学考虑因素的数学模型。

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