肺移植后巨细胞病毒感染和疾病的预防：采用延迟使用更昔洛韦的独特方案的结果

Prevention of cytomegalovirus infection and disease after lung transplantation: results using a unique regimen employing delayed ganciclovir.

作者信息

Brumble Lisa M, Milstone Aaron P, Loyd James E, Ely E Wesley, Pierson Richard N, Gautam Shiva, Dummer J Stephen

机构信息

Division of Infectious Diseases, Mayo Clinic, Jacksonville, FL, USA.

出版信息

Chest. 2002 Feb;121(2):407-14. doi: 10.1378/chest.121.2.407.

DOI:10.1378/chest.121.2.407

PMID:11834650

Abstract

BACKGROUND

Many lung transplant programs employ lengthy regimens of IV ganciclovir therapy to prevent disease due to cytomegalovirus (CMV). In 1994, we introduced a regimen of delayed ganciclovir prophylaxis for CMV infection. This consisted of 2 weeks of IV ganciclovir therapy, initiated 3 to 4 weeks after transplantation, with subsequent viral monitoring and preemptive therapy as needed. When not receiving ganciclovir, patients received oral acyclovir, 800 mg tid, for 6 months. CMV-seronegative patients with seropositive donors also received four doses of CMV hyperimmune globulin. This study analyzes the CMV outcomes of 54 patients who received the delayed regimen compared to 33 historical control subjects who received only acyclovir prophylaxis (n = 28) or oral acyclovir and 2 to 4 weeks of ganciclovir early after transplantation (n = 5).

METHODS

CMV detection was by shell vial culture or IgG seroconversion; after 1996, CMV detection was by blood antigenemia. The diagnosis of CMV disease also required a typical clinical syndrome or pathologic evidence of CMV. The main outcome was the actuarial incidence of CMV infection and disease. In order to account for the effect of other important risk factors for CMV infection, the time to CMV infection and disease was also studied as dependeant variables in a Cox proportional-hazard analysis, with the delayed regimen and other important risk factors as independent variables.

RESULTS

The delayed regimen reduced the actuarial incidence of CMV infection from 80 to 48% (p < 0.001) and CMV disease from 31 to 10% (p < 0.01). No seropositive patient receiving the delayed regimen developed CMV disease. Twelve of the 54 patients in the study group required additional IV antiviral treatment, but the total use of ganciclovir averaged only 18 days per patient. In a Cox proportional-hazards model, the use of delayed ganciclovir was the only factor that showed a significant association with freedom from CMV infection (hazard ratio [HR], 0.43; 95% confidence interval [CI], 0.24 to 0.75; p = 0.003) and CMV disease (HR, 0.29; 95% CI, 0.10 to 0.86; p = 0.03).

CONCLUSION

A regimen of CMV prophylaxis employing 2 weeks of IV ganciclovir initiated 3 to 4 weeks after lung transplantation followed by virologic monitoring and preemptive therapy as needed provides good protection against CMV disease.

摘要

背景

许多肺移植项目采用长时间的静脉注射更昔洛韦疗法来预防巨细胞病毒（CMV）感染所致疾病。1994年，我们引入了一种针对CMV感染的延迟更昔洛韦预防方案。该方案包括在移植后3至4周开始进行2周的静脉注射更昔洛韦治疗，随后根据需要进行病毒监测和抢先治疗。在未接受更昔洛韦治疗时，患者口服阿昔洛韦，800毫克，每日三次，持续6个月。供体血清反应阳性的CMV血清反应阴性患者还接受四剂CMV高效价免疫球蛋白治疗。本研究分析了54例接受延迟方案患者的CMV感染结果，并与33例历史对照受试者进行比较，这些对照受试者仅接受阿昔洛韦预防（n = 28）或口服阿昔洛韦以及移植后早期2至4周的更昔洛韦治疗（n = 5）。

方法

通过空斑试验培养或IgG血清转化检测CMV；1996年后，通过血液抗原血症检测CMV。CMV疾病的诊断还需要典型的临床综合征或CMV的病理证据。主要结局是CMV感染和疾病的精算发病率。为了考虑CMV感染其他重要危险因素的影响，在Cox比例风险分析中，将CMV感染和疾病的发生时间作为因变量进行研究，将延迟方案和其他重要危险因素作为自变量。

结果

延迟方案将CMV感染的精算发病率从80%降至48%（p < 0.001），将CMV疾病的发病率从31%降至10%（p < 0.01）。接受延迟方案的血清反应阳性患者均未发生CMV疾病。研究组的54例患者中有12例需要额外的静脉抗病毒治疗，但更昔洛韦的总使用量平均每位患者仅18天。在Cox比例风险模型中，使用延迟更昔洛韦是唯一与免于CMV感染（风险比[HR]，0.43；95%置信区间[CI]，0.24至0.75；p = 0.003）和CMV疾病（HR，0.29；95%CI，0.10至0.86；p = 0.03）显著相关的因素。