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即使高剂量的延长输注也可能无法达到所需的β-内酰胺浓度:治疗药物监测的价值。

Even high-dose extended infusions may not yield desired concentrations of β-lactams: the value of therapeutic drug monitoring.

机构信息

From the Burns Trauma and Critical Care Research Centre, University of Queensland , Queensland , Australia.

出版信息

Infect Dis (Lond). 2015;47(10):739-42. doi: 10.3109/23744235.2015.1021831. Epub 2015 Mar 10.

Abstract

A 35-year-old patient in intensive care with severe burn injury developed episodes of sepsis. Blood culture yielded a multidrug-resistant Pseudomonas aeruginosa and treatment was commenced with amikacin (minimum inhibitory concentration (MIC) 2-4 mg/L, dose 20 mg/kg adjusted body weight 24-hourly) and meropenem (MIC 8 mg/L, dose 2 g IV 8-hourly and later 6-hourly). Despite the use of extended infusions with β-lactam therapeutic drug monitoring and doses that were more than 2.5 times higher than standard meropenem doses, resistance emerged. This case report describes the application of therapeutic drug monitoring to optimize β-lactam therapy in a difficult-to-treat critically ill patient.

摘要

一位 35 岁的重症监护烧伤患者发生脓毒症发作。血培养检出多重耐药铜绿假单胞菌,开始用阿米卡星(最小抑菌浓度(MIC)2-4mg/L,剂量 20mg/kg 调整体重量 24 小时一次)和美罗培南(MIC8mg/L,剂量 2g IV 每 8 小时一次,后来每 6 小时一次)治疗。尽管使用了β-内酰胺治疗药物监测的延长输注和超过标准美罗培南剂量 2.5 倍以上的剂量,但仍出现耐药性。本病例报告描述了应用治疗药物监测来优化治疗药物监测在难以治疗的危重病患者中的β-内酰胺治疗。

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