无环鸟苷治疗新生儿和儿童单纯疱疹病毒感染肾毒性风险的临床回顾

Nahed O. ElHassan, Brendan Crawford, Zain Alamarat, Jacob T. Painter
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引用次数: 0

摘要

目的:本研究旨在阐明静脉使用阿昔洛韦(ACV)治疗单纯疱疹病毒(HSV)感染的新生儿(年龄3个月)和儿童(年龄≥3个月至12岁)的肾毒性风险,并确定可进一步研究的知识空白。方法检索多个数据库,以确定ACV用于治疗侵袭性HSV感染(定义为任何新生儿感染或儿童HSV脑炎(HSE))的肾毒性风险的研究。结果分别有5项和14项研究评估了新生儿和儿童acv相关肾毒性的风险。美国食品和药物管理局(FDA)推迟了对high (HD;60 mg/kg/天)ACV对新生儿继发毒性风险。根据我们的综述,与儿科人群相比,新生儿acv相关肾毒性的风险较低。阿昔洛韦剂量(1500mg /m2)、年龄和同时使用肾毒性药物被确定为增加儿童ACV肾毒性风险的变量。虽然FDA已经批准使用HD ACV治疗儿童HSE,但美国儿科学会建议使用较低的剂量以尽量减少毒性风险。高剂量与低剂量ACV对儿童HSE管理的有效性和安全性尚待评估。结论:与年龄较大的儿童相比,新生儿acv相关肾毒性的风险较低。未来的研究需要确定ACV在HSE患儿中最大限度降低毒性和最大限度提高疗效的最佳剂量。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Clinical Review of Risk of Nephrotoxicity with Acyclovir Use for Treatment of Herpes Simplex Virus Infections in Neonates and Children
OBJECTIVE This study aims to clarify the risk of nephrotoxicity with intravenous use of acyclovir (ACV) for the treatment of neonates (ages <3 months) and children (ages ≥3 months to <12 years) with herpes simplex virus (HSV) infections and to identify gaps in knowledge that could be further investigated. METHODS Multiple databases were searched to identify studies on risk of nephrotoxicity with ACV use for treatment of invasive HSV infections, defined as any neonatal infection or HSV encephalitis (HSE) in children. RESULTS There were 5 and 14 studies that evaluated the risk of ACV-associated nephrotoxicity in neonates and children, respectively. The US Food and Drug Administration (FDA) delayed the approval of high (HD; 60 mg/kg/day) ACV in neonates secondary to risk of toxicity. Based on our review, the risk of ACV-associated nephrotoxicity was lower in the neonatal compared with the pediatric population. Acyclovir dose >1500 mg/m2, older age, and concomitant use of nephrotoxic drugs were identified as variables that increased the risk of ACV nephrotoxicity in children. Although the FDA has approved the use of HD ACV for the treatment of HSE in children, the American Academy of Pediatrics recommends a lower dose to minimize the risk of toxicity. The efficacy and safety of high vs lower doses of ACV for the management of HSE in children has yet to be evaluated. CONCLUSIONS The risk of ACV-associated nephrotoxicity was lower among neonates compared with older children. Future studies are needed to identify the optimal dosage that minimizes toxicities and maximizes the efficacy of ACV in children with HSE.
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