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简介:来氟米特和药代动力学/药效学原理支持来氟米特的剂量选择。

Introduction: lefamulin and pharmacokinetic/pharmacodynamic rationale to support the dose selection of lefamulin.

机构信息

University of Illinois at Chicago, Colleges of Pharmacy and Medicine, Chicago, IL, USA.

出版信息

J Antimicrob Chemother. 2019 Apr 1;74(Suppl 3):iii2-iii4. doi: 10.1093/jac/dkz084.

Abstract

Lefamulin is the first semisynthetic pleuromutilin being developed for oral and intravenous administration. The drug selectively inhibits prokaryotic ribosomal protein synthesis by binding to the peptidyl transferase centre via four H-bonds and other interactions, resulting in an 'induced fit' that tightens the binding pocket around lefamulin. This unique mechanism of action has been associated with a low probability of cross-resistance to other antimicrobial classes commonly used to treat community-acquired bacterial pneumonia (CABP). This Supplement, entitled 'Pharmacokinetic and pharmacodynamic analyses and dose rationale for lefamulin, a novel pleuromutilin antibiotic, for the treatment of community-acquired bacterial pneumonia', is intended to be a valuable resource for both clinicians and researchers. It provides the essential pharmacokinetic and pharmacodynamic data on lefamulin that were used to support the optimal dose selection of lefamulin for the safe and effective treatment of CABP in adults.

摘要

lefamulin 是首个正在开发的用于口服和静脉给药的半合成截短侧耳素。该药物通过与肽基转移酶中心的四个氢键和其他相互作用结合,选择性地抑制原核核糖体蛋白合成,导致“诱导契合”,从而使 lefamulin 周围的结合口袋变紧。这种独特的作用机制与其他常用于治疗社区获得性细菌性肺炎 (CABP) 的抗菌药物类别发生交叉耐药的可能性较低有关。本增刊题为“新型截短侧耳素抗生素 lefamulin 的药代动力学和药效学分析及剂量合理性,用于治疗社区获得性细菌性肺炎”,旨在为临床医生和研究人员提供有价值的资源。它提供了 lefamulin 的基本药代动力学和药效学数据,这些数据用于支持 lefamulin 的最佳剂量选择,以安全有效地治疗成人 CABP。

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