Once-a-day administration of amikacin in neonates: assessment of nephrotoxicity and ototoxicity.

J P Langhendries, O Battisti, J M Bertrand, A François, J Darimont, S Ibrahim, P M Tulkens, A Bernard, J P Buchet, E Scalais
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引用次数: 57

Abstract

Neonates, especially preterms, are known to have low glomerular filtration rates (GFR). This may result in elevated trough concentrations during multiple administration of aminoglycosides (AGs), potentially leading to nephro- and ototoxic reactions. The once-daily administration (q.d.) of AGs has been shown to be equally or better tolerated in adults and children than the conventional schedules (twice daily, b.i.d.; thrice daily, t.i.d.), while offering potential pharmacodynamic and nursing advantages. No data, however, are available for neonates. As a consequence, this pilot study was conducted in order to assess the tolerance of the once-a-day administration of amikacin in comparison with the twice daily dose regimen, in relation to the pharmacokinetics of the drug under these two schedules. 22 Male neonates (gestational age > or = 34 weeks; postnatal age < or = 2 days) were randomized to receive amikacin (AK) (15 mg/kg/day) q.d. (n = 10) or b.i.d. (n = 12) together with ampicillin (50 mg/kg/12 h). AK plasma levels were measured at days 1, 3, 5 and 7 of treatment just before the next dose (trough level) and 1 h after completion of infusion (peak level) and after 3 and 6 h only at day 1. Due to the small size of the samples, no difference in efficacy could be assessed and was not the aim per se. Glomerular dysfunction was assessed by creatinine clearance, and tubular injuries by the urinary excretion of proteins (retinol binding protein, beta 2-microglobulin, clara cell protein (P1) and microalbumin), enzymes (N-acetyl-beta-D-glucosaminidase, alkaline phosphatase, alanine aminopeptidase, and gamma-glutamyltransferase), and total phospholipids (TPL) in urine. Ototoxicity was assessed by brainstem auditory evoked potentials (BAEPs) at days 0, 3 and 9 of therapy. Eight healthy neonates served as controls. All patients showed a normal and similar increase of GFR during the first postnatal days. Proteinuria did not increase, but enzymuria and TPL increased significantly during the treatment in both AK groups without significant difference between groups. BAEPs at day 9 were not significantly different between treated and untreated patients. We conclude from this pilot study that, in the absence of more toxicity, the q.d. administration of AK in neonates of > or = 34 weeks of gestational age may be recommended over its bid schedule in view of its potential advantages.

新生儿每日一次阿米卡星:肾毒性和耳毒性评估。
新生儿,尤其是早产儿,肾小球滤过率(GFR)较低。这可能导致多次给药氨基糖苷(AGs)时谷浓度升高,可能导致肾毒性和耳毒性反应。每日一次给药(q.d)已被证明在成人和儿童中与传统的时间表(每日两次,b.i.d;每日三次,t.i.d),同时提供潜在的药效学和护理优势。然而,没有关于新生儿的数据。因此,进行这项初步研究是为了评估每天一次给药阿米卡星与每天两次给药方案的耐受性,以及这两种方案下药物的药代动力学。男婴22例(胎龄>或= 34周);出生年龄<或= 2天)随机接受阿米卡星(AK) (15 mg/kg/天)每日一次(n = 10)或每日一次(n = 12)与氨苄西林(50 mg/kg/12小时)联合治疗。在治疗的第1、3、5和7天(下一剂量前)和输注完成后1小时(峰值水平)以及第1天3和6小时后测量AK血浆水平。由于样本量小,无法评估疗效的差异,也不是目的本身。通过肌酐清除率评估肾小球功能障碍,通过尿中蛋白质(视黄醇结合蛋白、β 2-微球蛋白、克拉拉细胞蛋白(P1)和微量白蛋白)、酶(n -乙酰- β - d -氨基葡萄糖苷酶、碱性磷酸酶、丙氨酸氨基肽酶和γ -谷氨酰转移酶)和总磷脂(TPL)的排泄来评估肾小球损伤。在治疗第0、3、9天采用脑干听觉诱发电位(BAEPs)评估耳毒性。8名健康新生儿作为对照。所有患者在出生后最初几天均表现出正常且相似的GFR升高。两组患者在治疗过程中蛋白尿均未增加,但酶血症和TPL均显著增加,两组间差异无统计学意义。第9天baep在治疗组和未治疗组之间无显著差异。我们从这项初步研究中得出结论,在没有更多毒性的情况下,考虑到其潜在的优势,在>或= 34周胎龄的新生儿中,可以推荐定量给药AK,而不是其投标时间表。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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