两种利奈唑胺剂量方案在耐多药和广泛耐药结核病患者中的药代动力学比较。
Comparison of the pharmacokinetics of two dosage regimens of linezolid in multidrug-resistant and extensively drug-resistant tuberculosis patients.
机构信息
Department of Hospital and Clinical Pharmacy and Toxicology, University Medical Center Groningen, University of Groningen, Groningen, the Netherlands.
出版信息
Clin Pharmacokinet. 2010 Aug;49(8):559-65. doi: 10.2165/11532080-000000000-00000.
BACKGROUND AND OBJECTIVES
For the treatment of multidrug-resistant (MDR) and extensively drug-resistant (XDR) tuberculosis (TB), potent new drugs are urgently needed. Linezolid is a promising drug, but its use is limited by adverse effects with prolonged administration of 600 mg twice daily. In order to reduce its adverse effects and maintain efficacy, we investigated whether linezolid in a reduced dosage resulted in drug serum concentrations exceeding a ratio of the in vitro minimum inhibitory concentration (MIC) to the area under the serum concentration-time curve (AUC) over 24 hours (AUC(24)) [AUC(24)/MIC] of >100.
PATIENTS AND METHODS
This open-label, prospective pharmacokinetic study evaluated two doses (300 and 600 mg) of linezolid in MDR-TB patients, who received linezolid as part of their treatment. They received linezolid 300 mg twice daily for 3 days, followed by 600 mg twice daily. Blood samples taken at predefined intervals for measuring serum linezolid concentrations were processed by a validated liquid chromatography-tandem mass spectrometry procedure. The AUC(24)/MIC ratio was used as a predictive model of efficacy. Adverse effects of linezolid, including peripheral neuropathy, were evaluated by clinical and laboratory assessments.
RESULTS
Eight patients were included in this study. The median duration of linezolid treatment was 56 days (interquartile range [IQR 44-82] days), with a median cumulative dose of 51,000 mg (IQR 33,850-60,450 mg). The median linezolid AUC over 12 hours (AUC(12)) values were 57.6 mg x h/L (IQR 38.5-64.2 mg x h/L) with the 300 mg dose and 145.8 mg x h/L (IQR 101.2-160.9 mg x h/L) with the 600 mg dose. The AUC(24)/MIC ratios were 452 (IQR 343-513) with the 300 mg dose and 1151 (IQR 656-1500) with the 600 mg dose. Linezolid was well tolerated.
CONCLUSION
Seemingly effective serum concentrations were reached after 3 days of administration of linezolid 300 mg twice daily, i.e. the AUC(24)/MIC ratio was at least 100 in 7 of 8 patients. Larger numbers of patients should be studied to confirm the efficacy of the linezolid 300 mg twice-daily dosage in MDR-TB or XDR-TB treatment.
背景与目的
对于耐多药(MDR)和广泛耐药(XDR)结核病(TB)的治疗,迫切需要新的有效药物。利奈唑胺是一种有前途的药物,但由于每日两次服用 600 毫克的不良反应限制了其使用。为了降低不良反应并保持疗效,我们研究了利奈唑胺的低剂量是否会导致药物血清浓度超过体外最低抑菌浓度(MIC)与 24 小时血清浓度-时间曲线下面积(AUC)的比值(AUC(24))[AUC(24)/MIC]超过 100。
患者和方法
这项开放标签、前瞻性药代动力学研究评估了 MDR-TB 患者中两种剂量(300 和 600 毫克)的利奈唑胺,他们将利奈唑胺作为治疗的一部分。他们先接受利奈唑胺 300 毫克,每日两次,持续 3 天,然后改为 600 毫克,每日两次。在预定义的时间间隔内采集血样以测量血清利奈唑胺浓度,并通过经过验证的液相色谱-串联质谱程序进行处理。AUC(24)/MIC 比值被用作疗效的预测模型。通过临床和实验室评估评估了利奈唑胺的不良反应,包括周围神经病。
结果
这项研究纳入了 8 名患者。利奈唑胺治疗的中位持续时间为 56 天(四分位距 [IQR] 44-82 天),累积剂量中位数为 51000 毫克(IQR 33850-60450 毫克)。300 毫克剂量的 AUC(12)中位值为 57.6mg·h/L(IQR 38.5-64.2mg·h/L),600 毫克剂量的 AUC(12)中位值为 145.8mg·h/L(IQR 101.2-160.9mg·h/L)。AUC(24)/MIC 比值分别为 300 毫克剂量组的 452(IQR 343-513)和 600 毫克剂量组的 1151(IQR 656-1500)。利奈唑胺耐受性良好。
结论
在每日两次服用 300 毫克利奈唑胺 3 天后,似乎达到了有效的血清浓度,即 8 名患者中有 7 名的 AUC(24)/MIC 比值至少为 100。需要更多的患者来证实每日两次 300 毫克利奈唑胺剂量在 MDR-TB 或 XDR-TB 治疗中的疗效。
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