Halacová M, Průsa R, Kotaska K, Vávrová V
Ustav klinické biochemie a patobiochemie 2. LF UK a FNM, Praha.
Cas Lek Cesk. 2004;143(3):187-90.
Once-daily administration of aminoglykosides is routinely used, but comparative efficacy data for patients with cystic fibrosis are not available.
The aim of the this study was to compare the predicted pharmacodynamic (PD) activity of amikacin at 28 mg/kg/den administered every 24 hod.(q24h), q12h, and q8h. Pharmacokinetic (PK) data were derived from analysis of the amikacin serum concentration from 42 CF children patients. Individual pharmacokinetics values were used to construct serum concentration--versus time curves and to determine various indices (c peak/MIC ratio and time during the concentration was less than the MIC--T < MIC) for all three dose regimens described above. MIC (minimal inhibitory concentration) for Pseudomonas aeruginosa was 4 mg/l. Significantly lower c peak/MIC but shorter T < MIC were noted when regimens of q8h versus q12h (p < 0.001), q8h vs. q24h (p < 0.001) and q12h vs. q24h (p < 0.001) were compared. This analysis suggests that the potential advantage of achieving a greater c peak/MIC with once-daily aminoglycoside administration may be neutralized by the significantly greater T < MIC in CF patients compared with that achieved with multiple-daily-dosing regimens.
Routine use of once daily amikacin administration could not be recommended until the clinical data confirming efficiency of this dose modality are available.
氨基糖苷类药物每日一次给药已常规使用,但囊性纤维化患者的比较疗效数据尚不可得。
本研究的目的是比较阿米卡星在每24小时(q24h)、q12h和q8h给予28mg/kg/日时预测的药效学(PD)活性。药代动力学(PK)数据来自对42例囊性纤维化儿童患者的阿米卡星血清浓度分析。个体药代动力学值用于构建血清浓度-时间曲线,并确定上述三种给药方案的各种指标(c峰/MIC比值以及浓度低于MIC的时间-T<MIC)。铜绿假单胞菌的MIC(最低抑菌浓度)为4mg/l。当比较q8h与q12h(p<0.001)、q8h与q24h(p<0.001)以及q12h与q24h(p<0.001)的给药方案时,发现c峰/MIC显著降低,但T<MIC较短。该分析表明,与多次给药方案相比,囊性纤维化患者中每日一次给予氨基糖苷类药物实现更高c峰/MIC的潜在优势可能会被显著更长的T<MIC所抵消。
在获得证实这种给药方式有效性的临床数据之前,不建议常规使用每日一次的阿米卡星给药。
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