使用高剂量(≥8毫克/千克)达托霉素治疗时的安全性和临床结果。
Safety and clinical outcomes when utilizing high-dose (> or =8 mg/kg) daptomycin therapy.
作者信息
Moise Pamela A, Hershberger Ellie, Amodio-Groton Maria I, Lamp Kenneth C
机构信息
Cubist Pharmaceuticals Inc., Lexington, MA 02421, USA.
出版信息
Ann Pharmacother. 2009 Jul;43(7):1211-9. doi: 10.1345/aph.1M085. Epub 2009 Jul 7.
BACKGROUND
Daptomycin is approved for the treatment of skin and skin-structure infections (4 mg/kg) and Staphylococcus aureus bacteremia, including right-sided endocarditis (6 mg/kg). In vitro and animal studies have reported increased activity with increased daptomycin doses. There are limited clinical data on use of daptomycin at doses greater than 6 mg/kg.
OBJECTIVE
To evaluate the safety and efficacy of higher doses (> or =8 mg/kg) of daptomycin when administered for a variety of gram-positive infections.
METHODS
Data were collected retrospectively as part of an ongoing registry (the Cubicin Outcomes Registry and Experience database) for the 2005-2007 program years. For the purpose of this study, the safety and efficacy of daptomycin were evaluated in patients who received doses of 8 mg/kg or higher.
RESULTS
Ninety-four (2.6%) of 3617 patients received daptomycin doses of 8 mg/kg or higher; 18 (19%) of those patients received doses of 10 mg/kg or higher. The most common infections were bacteremia (30/94), skin and skin-structure infections (22/94), and endocarditis (15/94). The most common pathogens were Enterococcus spp. (37/94; 57% vancomycin-resistant) and S. aureus (28/94; 68% methicillin-resistant). Fifty-one percent of the patients were male, 39% were aged 66 years or older, 27% had an initial creatinine clearance less than 30 mL/min, and 17% were on dialysis. The median duration of daptomycin therapy was 15 days (minimum 1, maximum 90). Six (6.4%) of the 94 patients experienced 1 or more adverse events or abnormal laboratory value changes possibly related to daptomycin; in 2 (2.1%) of the 94 patients, daptomycin was discontinued due to treatment-related adverse events. Seventy-four (79%) patients were considered evaluable for efficacy. The overall clinical success rate was 89% (bacteremia, 91%; skin and skin-structure infections, 88%; endocarditis, 67%).
CONCLUSIONS
Daptomycin was well tolerated and effective at doses of 8 mg/kg or higher in patients with gram-positive infections. Further prospective and comparative studies of daptomycin at doses greater than 6 mg/kg are warranted.
背景
达托霉素已被批准用于治疗皮肤及皮肤结构感染(4毫克/千克)以及金黄色葡萄球菌血症,包括右侧心内膜炎(6毫克/千克)。体外及动物研究报告称,达托霉素剂量增加时活性增强。关于使用大于6毫克/千克剂量达托霉素的临床数据有限。
目的
评估更高剂量(≥8毫克/千克)的达托霉素用于多种革兰氏阳性菌感染时的安全性和疗效。
方法
作为2005 - 2007项目年度正在进行的注册研究( Cubicin结果注册与经验数据库)的一部分,回顾性收集数据。为了本研究的目的,对接受8毫克/千克或更高剂量达托霉素的患者的安全性和疗效进行评估。
结果
3617例患者中有94例(2.6%)接受了8毫克/千克或更高剂量的达托霉素;其中18例(19%)患者接受了10毫克/千克或更高剂量。最常见的感染为菌血症(30/94)、皮肤及皮肤结构感染(22/94)和心内膜炎(15/94)。最常见的病原体为肠球菌属(37/94;57%对万古霉素耐药)和金黄色葡萄球菌(28/94;68%对甲氧西林耐药)。51%的患者为男性,39%的患者年龄在66岁及以上,27%的患者初始肌酐清除率低于30毫升/分钟,17%的患者正在接受透析。达托霉素治疗的中位持续时间为15天(最短1天,最长90天)。94例患者中有6例(6.4%)发生了1次或更多次可能与达托霉素相关的不良事件或实验室值异常变化;94例患者中有2例(2.1%)因治疗相关不良事件停用达托霉素。74例(79%)患者被认为可评估疗效。总体临床成功率为89%(菌血症,91%;皮肤及皮肤结构感染,88%;心内膜炎,67%)。
结论
对于革兰氏阳性菌感染患者,8毫克/千克或更高剂量的达托霉素耐受性良好且有效。有必要对大于6毫克/千克剂量的达托霉素进行进一步的前瞻性和对比研究。
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