Department of Basic and Clinical Pharmacology, School of Pharmacy, Anhui Medical Universitygrid.186775.a, Hefei, China.
Anhui Province Key Laboratory of Major Autoimmune Diseases, School of Pharmacy, Anhui Institute of Innovative Drugs, Anhui Medical Universitygrid.186775.a, Hefei, China.
Microbiol Spectr. 2021 Dec 22;9(3):e0087121. doi: 10.1128/Spectrum.00871-21. Epub 2021 Dec 1.
The rapid spread of antibiotic resistance among has prompted considerable interest in determining the dosage regimen of linezolid combined with fosfomycin. A checkerboard assay was employed to evaluate whether linezolid combined with fosfomycin had a synergistic effect on isolates from the hospital, including three drug-resistant strains (MIC of linezolid [MIC], ≥8 mg/L; MIC of fosfomycin [MIC], ≥256 mg/L). The static time-kill assay, dynamic pharmacokinetic (PK)/pharmacodynamic (PD) model, and semimechanistic PK/PD model were used to explore and predict effective combined dosage regimens. The checkerboard assay and static time-kill assay demonstrated that linezolid combined with fosfomycin has a synergistic effect on drug-resistant and sensitive . In the PK/PD model, the dosage regimen of linezolid (8 mg/L or 12 mg/L, steady-state concentration) combined with fosfomycin (6 g or 8 g) via a 0.5-h infusion every 8 h effectively suppressed bacterial growth at 24 h with a 3 log CFU/mL decrease compared with the initial inocula against two resistant and one sensitive isolates. The semimechanistic PK/PD model predicted that linezolid (more than 16 mg/L) combined with fosfomycin (6 g or 10 g) via a 0.5-h infusion every 8 h was required to achieve a 4 log CFU/mL decrease at 24 h against isolates (MIC ≥ 8 mg/L and MIC ≥ 256 mg/L). According to the prediction of the semimechanical PK/PD model, the effect of the combination was driven by linezolid, with fosfomycin enhancing the effect. Our study is the first to explore the synergistic effects of these two drugs from a qualitative and quantitative perspective and provides a simulation tool for future studies. In this study, we found that linezolid combined with fosfomycin could kill and that the administered dose was significantly lower after the combination treatment, which could reduce adverse effects and the development of drug resistance. The potential mechanism of the two-drug combination against was revealed from a quantitative perspective, which is an important step toward dose optimization in simulated humans. We hope that our research will help build a better relationship between clinicians and patients as we work together to address the challenges of antibiotic resistance in the 21st century.
耐抗生素的 迅速传播促使人们非常关注确定利奈唑胺联合磷霉素的剂量方案。采用棋盘试验评估利奈唑胺联合磷霉素对来自医院的 分离株(包括 3 株耐药株,利奈唑胺 MIC[MIC]≥8mg/L;磷霉素 MIC[MIC]≥256mg/L)是否具有协同作用。采用 静态时间杀菌试验、动态药代动力学(PK)/药效动力学(PD)模型和半机械 PK/PD 模型来探索和预测有效的联合剂量方案。棋盘试验和 静态时间杀菌试验表明,利奈唑胺联合磷霉素对耐药和敏感 具有协同作用。在 PK/PD 模型中,利奈唑胺(8mg/L 或 12mg/L,稳态浓度)联合磷霉素(6g 或 8g)每 8 小时 0.5 小时输注的剂量方案可有效抑制 24 小时细菌生长,与初始接种物相比,两种耐药株和一株敏感株的细菌减少 3 log CFU/mL。半机械 PK/PD 模型预测,利奈唑胺(超过 16mg/L)联合磷霉素(6g 或 10g)每 8 小时 0.5 小时输注可在 24 小时内使 MIC≥8mg/L 和 MIC≥256mg/L 的 分离株的细菌减少 4 log CFU/mL。根据半机械 PK/PD 模型的预测,联合用药的效果由利奈唑胺驱动,磷霉素增强了这种效果。本研究首次从定性和定量角度探讨了这两种药物的协同作用,并为未来的研究提供了模拟工具。 在这项研究中,我们发现利奈唑胺联合磷霉素可以杀死 ,并且联合治疗后的给药剂量显著降低,这可以减少不良反应和耐药性的发展。从定量角度揭示了两药联合治疗 的潜在机制,这是在模拟人体中优化剂量的重要一步。我们希望我们的研究将有助于在临床医生和患者之间建立更好的关系,因为我们共同努力应对 21 世纪抗生素耐药性的挑战。
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