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通过一种新型细胞因子吸附剂系统在体外去除抗感染药物。

In vitro removal of anti-infective agents by a novel cytokine adsorbent system.

作者信息

König Christina, Röhr Anka C, Frey Otto R, Brinkmann Alexander, Roberts Jason A, Wichmann Dominic, Braune Stephan, Kluge Stefan, Nierhaus Axel

机构信息

1 Department of Intensive Care Medicine, University Medical Centre Hamburg-Eppendorf, Hamburg, Germany.

2 Hospital Pharmacy, University Medical Centre Hamburg-Eppendorf, Hamburg, Germany.

出版信息

Int J Artif Organs. 2019 Feb;42(2):57-64. doi: 10.1177/0391398818812601. Epub 2018 Dec 13.

Abstract

OBJECTIVES

: The aim of this study is to describe the in vitro adsorption of anti-infective drugs onto an extracorporeal cytokine adsorber.

METHODS

: Various anti-infective drugs (β-lactams, quinolones, aminoglycosides, glycopeptides, azole antimycotics) were prepared in normal saline 0.9% and human albumin 5%, and pumped through a cytokine cartridge (CytoSorb; CytoSorbents Corporation, Monmouth Junction, NJ, USA) at a flow rate of 1.2 L/h for 1.5 h. In addition, meropenem and ciprofloxacin were dissolved in reconstituted blood and run through a CytoSorb cartridge, which was integrated into a continuous renal replacement therapy circuit with a flow rate of 2 L/h for 18 h. Samples from the solution, pre- and post-filter, were quantified by high-performance liquid chromatography with ultraviolet detection and fluorescence polarisation immunoassay.

RESULTS

: Observed mean clearance of the drugs in normal saline was 1.22 ± 0.07 L/h. In human albumin, clearance was 1.29 ± 0.08 L/h. In reconstituted blood, clearance of meropenem decreased from 5.4 to 1.4 L/h and for ciprofloxacin from 6.3 to 4.3 L/h within the first 1.5 h because of early drug adsorption. Continuous renal replacement therapy clearance measured without CytoSorb was stable at 2 and 1.7 L/h, respectively. Approximately 400 mg of meropenem and 300 mg of ciprofloxacin had been adsorbed by CytoSorb, suggesting that these amounts are the maximum adsorptive capacity for these drugs.

CONCLUSION

: In these settings, all tested drugs were adsorbed by the cartridge in relevant amounts. The identified maximum adsorptive capacity and the rapid decline in concentration during the first 1.5 h of CytoSorb use suggest that the administration of an additional dose within the first hours of CytoSorb treatment may be reasonable. In addition, early therapeutic drug monitoring should be considered.

摘要

目的

本研究旨在描述抗感染药物在体外细胞因子吸附器上的吸附情况。

方法

将各种抗感染药物(β-内酰胺类、喹诺酮类、氨基糖苷类、糖肽类、唑类抗真菌药)分别溶于0.9%生理盐水和5%人白蛋白中,以1.2 L/h的流速泵入细胞因子吸附柱(CytoSorb;CytoSorbents公司,美国新泽西州蒙茅斯章克申),持续1.5小时。此外,将美罗培南和环丙沙星溶于复溶血液中,流经整合在持续肾脏替代治疗回路中的CytoSorb吸附柱,流速为2 L/h,持续18小时。通过带紫外检测的高效液相色谱法和荧光偏振免疫分析法对溶液、过滤器前后的样品进行定量分析。

结果

观察到药物在生理盐水中的平均清除率为1.22±0.07 L/h。在人白蛋白中,清除率为1.29±0.08 L/h。在复溶血液中,由于早期药物吸附,美罗培南的清除率在最初1.5小时内从5.4降至1.4 L/h,环丙沙星的清除率从6.3降至4.3 L/h。未使用CytoSorb时测得的持续肾脏替代治疗清除率分别稳定在2和1.7 L/h。CytoSorb吸附了约400 mg美罗培南和300 mg环丙沙星,表明这些量是这些药物的最大吸附容量。

结论

在这些条件下,所有测试药物均被吸附柱大量吸附。确定的最大吸附容量以及使用CytoSorb最初1.5小时内浓度的快速下降表明,在CytoSorb治疗的最初几小时内额外给药可能是合理的。此外,应考虑早期治疗药物监测。

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