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替加环素单独及联合治疗产 KPC 碳青霉烯酶肺炎克雷伯菌体外药效动力学研究

In vitro pharmacodynamics of simulated pulmonary exposures of tigecycline alone and in combination against Klebsiella pneumoniae isolates producing a KPC carbapenemase.

机构信息

Center for Anti-Infective Research and Development, Hartford Hospital, Hartford, CT 06102, USA.

出版信息

Antimicrob Agents Chemother. 2011 Apr;55(4):1420-7. doi: 10.1128/AAC.01253-10. Epub 2011 Jan 31.

Abstract

Multidrug-resistant Klebsiella pneumoniae strains that produce a serine carbapenemase (KPC) are emerging worldwide, with few therapeutic options that retain consistent susceptibility. The objective of this study was to determine the effect of combination therapy with tigecycline versus tigecycline alone against KPC-producing isolates (KPC isolates). An in vitro pharmacodynamic model was used to simulate adult steady-state epithelial lining fluid concentrations of tigecycline (50 mg every 12 h) given alone and in combination with either meropenem (2 g by 3-hour infusion every 8 h) or rifampin (600 mg every 12 h). Five KPC isolates with various phenotypic profiles were exposed over 48 h. Time-kill curves were constructed, and the areas under the bacterial killing and regrowth curves (AUBCs) were calculated. No regimens tested were able to maintain bactericidal reductions in CFU over 48 h. The AUBCs for tigecycline and meropenem monotherapies at 48 h ranged from 375.37 to 388.11 and from 348.62 to 383.83 (CFU-h/ml), respectively. The combination of tigecycline plus meropenem significantly reduced the AUBCs at 24 and 48 h for isolates with tigecycline MICs of ≤ 2 μg/ml and meropenem MICs of ≤ 16 μg/ml (P < 0.001) but added no additional activity when the meropenem MIC was 64 μg/ml (P = 0.5). Rifampin provided no additional reduction in CFU or AUBC over tigecycline alone (P = 0.837). The combination of tigecycline with high-dose, prolonged-infusion meropenem warrants further study as a potential treatment option for these multidrug-resistant organisms.

摘要

产丝氨酸碳青霉烯酶(KPC)的多药耐药肺炎克雷伯菌菌株正在全球范围内出现,治疗选择有限,且对这些菌株的敏感性保持一致。本研究的目的是确定替加环素联合治疗与替加环素单药治疗对产 KPC 分离株(KPC 分离株)的效果。使用体外药效动力学模型模拟替加环素(50 mg,每 12 小时一次)单独给药和与美罗培南(2 g,每 8 小时 3 小时输注一次)或利福平(600 mg,每 12 小时一次)联合给药时成人稳态上皮衬里液浓度。将具有不同表型谱的 5 种 KPC 分离株暴露于 48 小时。构建时间杀伤曲线,并计算细菌杀伤和再生长曲线下面积(AUBC)。没有一种测试方案能够在 48 小时内保持杀菌减少的 CFU。替加环素和美罗培南单药治疗 48 小时的 AUBC 分别为 375.37 至 388.11 和 348.62 至 383.83(CFU-h/ml)。替加环素与美罗培南联合应用可显著降低替加环素 MIC 值≤2μg/ml 和美罗培南 MIC 值≤16μg/ml 的分离株在 24 和 48 小时的 AUBC(P <0.001),但当美罗培南 MIC 值为 64μg/ml 时,无额外活性(P=0.5)。利福平单独使用替加环素不能进一步降低 CFU 或 AUBC(P=0.837)。替加环素与高剂量、延长输注美罗培南联合应用作为这些多药耐药生物的潜在治疗选择值得进一步研究。

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