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阿昔洛韦和水痘带状疱疹免疫球蛋白在实体器官移植受者中的应用。

Aciclovir and varicella-zoster-immunoglobulin in solid-organ transplant recipients.

机构信息

Department of Pediatrics, Medical University Innsbruck, Innsbruck, Austria.

出版信息

Pediatr Nephrol. 2011 May;26(5):663-73. doi: 10.1007/s00467-010-1666-z. Epub 2010 Nov 15.

Abstract

Clear recommendations for the management of acute varicella-zoster virus (VZV) infections for cases of significant exposure and the use of prophylactic drugs after solid-organ transplantation are missing due to the lack of evidence by prospective studies. Heterogeneity in patient groups, patient numbers, age groups, immunosuppressive regimens, timing, and dosage of aciclovir and/or varicella-zoster immunoglobulin (VZIG), pre-transplant vaccination or VZV wild-type infection and inconsistency of data make comparability of different studies impossible. Although the benefit of aciclovir and/or VZIG is uncertain in immunosuppressed children, prospective controlled double-blind studies are not feasible for ethical considerations as fatal cases with disseminating varicella disease are well known in these patient groups despite the use of aciclovir and/or VZIG, whereas severe side-effects of these drugs are rare. However, a reporting bias is likely as mainly severe or fatal cases might have been predominantly published or cases of successfully used aciclovir and/or VZIG in mild cases or in cases of breakthrough infections after vaccination. As neither VZIG prophylaxis nor treatment with intravenous aciclovir offers complete protection against severe VZV infection to immunosuppressed pediatric solid-organ transplant recipients, high priority should be given to vaccination against VZV prior to transplantation, and, most importantly, in their close contact persons. Clinical observations suggest that only assessment of humoral immunity together with cellular immunity may allow predication about protection in exposed patients.

摘要

由于前瞻性研究缺乏证据,对于有重大接触风险的病例以及实体器官移植后的预防性药物使用,目前缺乏明确的急性水痘带状疱疹病毒(VZV)感染管理建议。由于患者群体、患者数量、年龄组、免疫抑制方案、阿昔洛韦和/或水痘带状疱疹免疫球蛋白(VZIG)的时间和剂量、移植前疫苗接种或 VZV 野生型感染以及数据的不一致性,使得不同研究之间的可比性变得不可能。尽管在免疫抑制儿童中阿昔洛韦和/或 VZIG 的益处不确定,但由于这些患者群体中即使使用阿昔洛韦和/或 VZIG,仍有致命的播散性水痘疾病病例,因此出于伦理考虑,前瞻性对照双盲研究是不可行的,而这些药物的严重副作用却很少见。然而,由于主要是严重或致命的病例可能已经被主要发表,或者在轻度病例或疫苗接种后突破性感染的情况下成功使用了阿昔洛韦和/或 VZIG,因此可能存在报告偏倚。由于 VZIG 预防或静脉内阿昔洛韦治疗并不能为免疫抑制的儿科实体器官移植受者提供针对严重 VZV 感染的完全保护,因此应高度重视在移植前以及最重要的是在其密切接触者中接种 VZV 疫苗。临床观察表明,只有评估体液免疫和细胞免疫相结合,才能预测暴露患者的保护情况。

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