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利用三株铜绿假单胞菌和体外药效学模型,将24小时浓度-时间曲线下面积与最低抑菌浓度之比作为氟喹诺酮类抗菌效果的一般预测指标。

Twenty-four-hour area under the concentration-time curve/MIC ratio as a generic predictor of fluoroquinolone antimicrobial effect by using three strains of Pseudomonas aeruginosa and an in vitro pharmacodynamic model.

作者信息

Madaras-Kelly K J, Ostergaard B E, Hovde L B, Rotschafer J C

机构信息

College of Pharmacy, University of Minnesota, Minneapolis, USA.

出版信息

Antimicrob Agents Chemother. 1996 Mar;40(3):627-32. doi: 10.1128/AAC.40.3.627.

Abstract

Several investigators have suggested that the 24-h area under the concentration-time curve (AUC)/MIC ratio (AUC/MIC24 or AUIC24) can be used to make comparisons of antimicrobial activity between fluoroquinolone antibiotics. Limited data exist regarding the generic predictive ability of AUC/MIC24 for the antimicrobial effects of fluoroquinolones. The purposes of the present investigation were to determine if the AUC/MIC24 can be used as a generic outcome predictor of fluoroquinolone antibacterial activity and to determine if a similar AUC/MIC24 breakpoint can be established for different fluoroquinolones. Using an in vitro pharmacodynamic model, 29 duplicate concentration time-kill curve experiments simulated AUC/MIC24s ranging from 52 to 508 SIT-1.h (inverse serum inhibitory titer integrated over time) with ciprofloxacin or ofloxacin against three strains of Pseudomonas aeruginosa. Each 24-h experiment was performed in cation-supplemented Mueller-Hinton broth with a starting inoculum of 10(6) CFU/ml. At timed intervals cation-supplemented Mueller-Hinton broth samples were collected for CFU and fluoroquinolone concentration determinations. Transformation of bacterial counts into the cumulative bacterial effect parameter of the 24-h area under the effect curve (AUEC24) was performed for each concentration time-kill curve. Multivariate regression analysis was used to compare pharmacodynamic predictors (AUC/MIC24, 24-h AUC, peak concentration [Cmax] to MIC ratios [Cmax:MIC], etc.) with ln AUEC24. To identify threshold breakpoint AUC/MIC24s, AUEC24s were stratified by the magnitude of AUC/MIC24 into subgroups, which were analyzed for differences in antibacterial effect. The Kruskal-Wallis test and subsequent Tukey's multiple comparison test were used to determine which AUC/MIC subgroups were significantly different. Multiple regression analysis revealed that only AUC/MIC24 (r2 = 0.65) and MIC (r2 = 0.03) were significantly correlated with antibacterial effect. At similar AUC/MIC24s, yet different MICs, Cmaxs, or elimination half-lives, the AUEC24s were similar for both fluoroquinolones. The relationship between AUC/MIC24 and ln AUEC24 was best described by a sigmoidal maximal antimicrobial effect (Emax) model (r2 = 0.72; Emax = 9.1; AUC/MIC50 = 119 SIT-1.h; S = 2.01 [S is an exponent that reflects the degree of sigmoidicity]). Ciprofloxacin-bacteria AUC/MIC24 values of < 100 SIT-1.h were significantly different (P < 0.05) from the AUC/MIC24 values of > 100 SIT-1.h. An ofloxacin AUC/MIC24 of > 100 SIT-1.h and an AUC/MIC24 of < 100 SIT-1.h exhibited a trend toward a significant difference (P > 0.05 but < 0.1). The inverse relationship between drug exposure and MIC increase postexposure was described by a sigmoidal fixed Emax model (AUC/MIC24, r2 = 0.40; AUC/MIC50 = 95 SIT-1.h; S = 1.97; Cmax:MIC, r2 = 0.41; Cmax:MIC50 = 7.3; S = 2.01). These data suggest that AUC/MIC24 may be the most descriptive measurement of fluoroquinolone antimicrobial activity against P. aeruginosa, that ofloxacin and ciprofloxacin have similar AUC/MIC24 threshold breakpoints at approximately 100 SIT-1.h, that the concentration-dependent selection of resistant organisms may parallel the threshold breakpoint of the antimicrobial effect, and that AUC/MIC24 generically describes the antibacterial effects of different fluoroquinolones.

摘要

几位研究者提出,24小时浓度-时间曲线下面积(AUC)/最低抑菌浓度比值(AUC/MIC24或AUIC24)可用于比较氟喹诺酮类抗生素之间的抗菌活性。关于AUC/MIC24对氟喹诺酮类抗菌作用的一般预测能力的数据有限。本研究的目的是确定AUC/MIC24是否可作为氟喹诺酮类抗菌活性的一般结果预测指标,以及是否可为不同的氟喹诺酮类建立相似的AUC/MIC24断点。使用体外药效学模型,进行了29次重复的浓度-时间杀菌曲线实验,模拟了环丙沙星或氧氟沙星对三株铜绿假单胞菌的AUC/MIC24范围为52至508 SIT-1·h(随时间积分的血清抑菌效价倒数)。每个24小时实验均在添加阳离子的穆勒-欣顿肉汤中进行,起始接种量为10(6) CFU/ml。在设定的时间间隔收集添加阳离子的穆勒-欣顿肉汤样本,用于测定CFU和氟喹诺酮浓度。对每条浓度-时间杀菌曲线,将细菌计数转化为效应曲线下24小时面积的累积细菌效应参数(AUEC24)。使用多元回归分析比较药效学预测指标(AUC/MIC24、24小时AUC、峰浓度[Cmax]与最低抑菌浓度比值[Cmax:MIC]等)与ln AUEC24。为确定阈值断点AUC/MIC24,将AUEC24按AUC/MIC24的大小分层为亚组,分析各亚组抗菌效果的差异。使用Kruskal-Wallis检验及随后的Tukey多重比较检验来确定哪些AUC/MIC亚组存在显著差异。多元回归分析显示,仅AUC/MIC24(r2 = 0.65)和最低抑菌浓度(r2 = 0.03)与抗菌效果显著相关。在相似的AUC/MIC24下,但最低抑菌浓度、Cmax或消除半衰期不同时,两种氟喹诺酮类的AUEC24相似。AUC/MIC24与ln AUEC24之间的关系最好用S形最大抗菌效应(Emax)模型描述(r2 = 0.72;Emax = 9.1;AUC/MIC50 = 119 SIT-1·h;S = 2.01 [S是反映S形程度的指数])。环丙沙星-细菌的AUC/MIC24值<100 SIT-1·h与>100 SIT-1·h的AUC/MIC24值有显著差异(P < 0.05)。氧氟沙星AUC/MIC24>100 SIT-1·h与<100 SIT-1·h呈现出显著差异的趋势(P > 0.05但<0.1)。药物暴露与暴露后最低抑菌浓度增加之间的反比关系用S形固定Emax模型描述(AUC/MIC24,r2 = 0.40;AUC/MIC50 = 95 SIT-1·h;S = 1.97;Cmax:MIC,r2 = 0.41;Cmax:MIC50 = 7.3;S = 2.01)。这些数据表明,AUC/MIC24可能是氟喹诺酮类对铜绿假单胞菌抗菌活性的最具描述性的指标,氧氟沙星和环丙沙星在约100 SIT-1·h处有相似的AUC/MIC24阈值断点,耐药菌的浓度依赖性选择可能与抗菌效果的阈值断点平行,且AUC/MIC24可一般地描述不同氟喹诺酮类的抗菌效果。

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