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非达霉素:抗艰难梭菌感染的最新武器。

Fidaxomicin: the newest addition to the armamentarium against Clostridium difficile infections.

机构信息

Department of Pharmacy Practice, School of Pharmacy, Bouvé College of Health Sciences, Northeastern University, Boston, Massachusetts, USA.

出版信息

Clin Ther. 2012 Jan;34(1):1-13. doi: 10.1016/j.clinthera.2011.12.003.

Abstract

BACKGROUND

Fidaxomicin, a macrolide antibiotic, was the first medication for the management of Clostridium difficile infections (CDI) to be approved by the US Food and Drug Administration in more than 20 years.

OBJECTIVE

This article reviews published literature on fidaxomicin for management of CDI, including its chemistry, spectrum of activity, pharmacokinetic properties, pharmacodynamics, therapeutic efficacy, adverse events, dosing, administration, and pharmacoeconomic considerations.

METHODS

Pertinent English-language literature was reviewed through searches of MEDLINE, EMBASE, and BIOSIS from 1975 through September 2011. Reference lists of identified publications and published abstracts from the Interscience Conference on Antimicrobial Agents and Chemotherapy meetings were also reviewed. Search terms included, but were not limited to, fidaxomicin, difimicin, lipiarmycin, tiacumicin B, OPT-80, Clostridium spp, and diarrhea.

RESULTS

A total of 79 publications were identified and 10 were excluded; 6 review articles and 4 abstracts that were later published as articles. Fidaxomicin's in vitro profile is favorable compared with oral metronidazole and vancomycin, with minimum inhibitory concentrations against C difficile that are 2 dilutions lower. From the 2 published Phase III trials, fidaxomicin was deemed to be noninferior in the treatment of mild to moderate CDI compared with oral vancomycin. Recurrence rates for all strains of CDI were lower with fidaxomicin than vancomycin. Adverse events associated with fidaxomicin were similar to placebo, with nausea and vomiting being the most common. Although no pharmacoeconomic studies have compared fidaxomicin with metronidazole or vancomycin, the current price exceeds $2500 (US) per treatment course.

CONCLUSIONS

Reports suggest that fidaxomicin is noninferior to oral vancomycin in the treatment of mild or moderate CDI, although no published comparisons with metronidazole exist to date. Additionally, fidaxomicin improved outcomes compared with oral vancomycin in terms of rates of relapse and recurrent CDI, and in patients who might require concomitant antibiotics. Prospective, randomized studies comparing fidaxomicin with metronidazole in the treatment of mild or moderate CDI, as well as against vancomycin for severe CDI, should be undertaken to clarify the exact role of fidaxomicin in clinical practice.

摘要

背景

fidaxomicin 是一种大环内酯类抗生素,是 20 多年来美国食品和药物管理局首次批准用于治疗艰难梭菌感染(CDI)的药物。

目的

本文综述了已发表的关于 fidaxomicin 治疗 CDI 的文献,包括其化学、活性谱、药代动力学特性、药效学、治疗效果、不良反应、剂量、给药和药物经济学考虑。

方法

通过检索 1975 年至 2011 年 9 月期间的 MEDLINE、EMBASE 和 BIOSIS 中的英文文献,对相关文献进行了回顾。还查阅了鉴定出版物的参考文献列表和发表的抗微生物制剂和化疗会议摘要。检索词包括但不限于 fidaxomicin、difimicin、lipiarmycin、tiacumicin B、OPT-80、梭菌属和腹泻。

结果

共确定了 79 篇文献,其中 10 篇被排除在外;6 篇综述文章和 4 篇后来作为文章发表的摘要。与口服甲硝唑和万古霉素相比,fidaxomicin 的体外谱更为有利,对艰难梭菌的最低抑菌浓度低 2 倍。从 2 项已发表的 III 期试验中,与口服万古霉素相比,fidaxomicin 在治疗轻度至中度 CDI 方面被认为是非劣效的。所有 CDI 菌株的复发率均低于万古霉素。与 fidaxomicin 相关的不良反应与安慰剂相似,最常见的是恶心和呕吐。虽然尚未有药物经济学研究比较 fidaxomicin 与甲硝唑或万古霉素,但目前的价格超过 2500 美元(美国)/疗程。

结论

报告表明,在治疗轻度或中度 CDI 方面,fidaxomicin 与口服万古霉素非劣效,尽管迄今为止尚无与甲硝唑的发表比较。此外,与口服万古霉素相比,fidaxomicin 在复发和复发性 CDI 以及需要同时使用抗生素的患者方面改善了结局。应进行前瞻性、随机研究,比较 fidaxomicin 治疗轻度或中度 CDI 的甲硝唑以及严重 CDI 的万古霉素,以明确 fidaxomicin 在临床实践中的确切作用。

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