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头孢他啶/阿维巴坦和磷霉素组合在中空纤维感染模型中对多重耐药. 的药代动力学/药效学分析

Pharmacokinetic/pharmacodynamic analysis of ceftazidime/avibactam and fosfomycin combinations in an hollow fiber infection model against multidrug-resistant .

机构信息

Institute of Pharmacy, University of Hamburg , Hamburg, Germany.

Dynamic Team - EA 7380, Faculté de Santé, Université Paris-Est-Créteil Val-De-Marne , Créteil, France.

出版信息

Microbiol Spectr. 2024 Jan 11;12(1):e0331823. doi: 10.1128/spectrum.03318-23. Epub 2023 Dec 8.

Abstract

Mechanistic understanding of pharmacodynamic interactions is key for the development of rational antibiotic combination therapies to increase efficacy and suppress the development of resistances. Potent tools to provide those insights into pharmacodynamic drug interactions are semi-mechanistic modeling and simulation techniques. This study uses those techniques to provide a detailed understanding with regard to the direction and strength of the synergy of ceftazidime-avibactam and ceftazidime-fosfomycin in a clinical isolate expressing extended spectrum beta-lactamase (CTX-M-15 and TEM-4) and carbapenemase (OXA-244) genes. Enhanced killing effects in combination were identified as a driver of the synergy and were translated from static time-kill experiments into the dynamic hollow fiber infection model. These findings in combination with a suppression of the emergence of resistance in combination emphasize a potential clinical benefit with regard to increased efficacy or to allow for dose reductions with maintained effect sizes to avoid toxicity.

摘要

对药效相互作用的机制理解是开发合理的抗生素联合治疗方案以提高疗效和抑制耐药性发展的关键。有力的工具可以提供这些关于药效药物相互作用的见解,包括半机制建模和模拟技术。本研究使用这些技术,针对表达扩展谱β-内酰胺酶(CTX-M-15 和 TEM-4)和碳青霉烯酶(OXA-244)基因的临床分离株中头孢他啶-阿维巴坦和头孢他啶-磷霉素的协同作用的方向和强度提供了详细的理解。组合中的增强杀伤作用被确定为协同作用的驱动因素,并从静态时间杀伤实验转化为动态中空纤维感染模型。这些发现结合对组合中耐药性出现的抑制作用,强调了在提高疗效或允许减少剂量以保持疗效大小以避免毒性方面的潜在临床益处。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3a0a/10783110/28fbb9070f36/spectrum.03318-23.f001.jpg

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