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Worldwide Experience with the Use of Doripenem against Extended-Spectrum-β-Lactamase-Producing and Ciprofloxacin-Resistant Enterobacteriaceae: Analysis of Six Phase 3 Clinical Studies

机译:使用多瑞培南抗广谱β-内酰胺酶和环丙沙星耐药肠杆菌科的全球经验:六个3期临床研究的分析

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摘要

The worldwide increase in fluoroquinolone-resistant and extended-spectrum β-lactamase (ESBL)-producing Enterobacteriaceae pathogens has led to doripenem and other carbapenems assuming a greater role in the treatment of serious infections. We analyzed data from 6 phase 3 multinational doripenem clinical trials on ciprofloxacin-resistant Enterobacteriaceae isolates consisting of all genera (CIPRE) and ESBL-producing Enterobacteriaceae isolates consisting of Escherichia coli, Klebsiella spp., and Proteus spp. with ceftazidime MICs of ≥2 μg/ml (ESBLE) for prevalence by geographic region and disease type, in vitro activities of doripenem and comparator agents, and clinical or microbiologic outcomes in doripenem- and comparator-treated patients across disease types (complicated intra-abdominal infection [cIAI], complicated urinary tract infection [cUTI], and nosocomial pneumonia [NP]). Of 1,830 baseline Enterobacteriaceae isolates, 88 (4.8%) were ESBLE and 238 (13.0%) were CIPRE. The incidence of ESBLE was greatest in Europe (7.8%); that of CIPRE was higher in South America (15.9%) and Europe (14.4%). ESBLE incidence was highest in NP (12.9%) cases; that of CIPRE was higher in cUTI (18.3%) and NP (14.9%) cases. Against ESBLE and CIPRE, carbapenems appeared more active than other antibiotic classes. Among carbapenems, doripenem and meropenem were most potent. Doripenem had low MIC90s for CIPRE (0.5 μg/ml) and ESBLE (0.25 μg/ml). Doripenem and comparators were highly clinically effective in infections caused by Enterobacteriaceae, irrespective of their ESBL statuses. The overall cure rates were the same for doripenem (82%; 564/685) and the comparators (82%; 535/652) and similar for ESBLE (73% [16/22] versus 72% [21/29]) and CIPRE (68% [47/69] versus 52% [33/64]). These findings indicate that doripenem is an important therapeutic option for treating serious infections caused by ESBLE and CIPRE.
机译:产生氟喹诺酮耐药和广谱β-内酰胺酶(ESBL)的肠杆菌科细菌病原体的全球增加已导致多立培南和其他碳青霉烯类在严重感染的治疗中发挥更大作用。我们分析了耐环丙沙星肠杆菌科细菌的6个3期跨国多瑞培南临床试验的数据,这些细菌由所有属(CIPRE)和产ESBL肠杆菌科细菌组成,包括大肠杆菌,克雷伯菌属和变形杆菌。头孢他啶MIC≥2μg/ ml(ESBLE),按地理区域和疾病类型,多瑞培南和比较剂的体外活性以及多瑞培南和比较剂治疗的患者在不同疾病类型中的临床或微生物学结局(复杂的腹部感染[cIAI],复杂的尿路感染[cUTI]和医院内肺炎[NP])。在1,830株基线肠杆菌科细菌中,ESBLE为88(4.8%),CIPRE为238(13.0%)。欧洲ESBLE的发生率最高(7.8%);南美洲(15.9%)和欧洲(14.4%)的CIPRE较高。 ESBLE发生率在NP病例中最高(12.9%); cUTI(18.3%)和NP(14.9%)病例的CIPRE较高。在对抗ESBLE和CIPRE方面,碳青霉烯类似乎比其他抗生素类更具活性。在碳青霉烯中,多立培南和美罗培南最有效。多瑞培南的CIPRE(0.5μg/ ml)和ESBLE(0.25μg/ ml)的MIC90较低。无论其ESBL状态如何,多瑞培南和比较剂在肠杆菌科细菌感染中均具有很高的临床疗效。多利培南的总治愈率是相同的(82%; 564/685)和比较者(82%; 535/652),而ESBLE的总治愈率相似(73%[16/22]对72%[21/29]), CIPRE(68%[47/69]对52%[33/64])。这些发现表明多利培南是治疗由ESBLE和CIPRE引起的严重感染的重要治疗选择。

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