口服更昔洛韦或口服阿昔洛韦预防器官移植受者原发性巨细胞病毒病
Prevention of primary cytomegalovirus disease in organ transplant recipients with oral ganciclovir or oral acyclovir prophylaxis.
作者信息
Rubin R H, Kemmerly S A, Conti D, Doran M, Murray B M, Neylan J F, Pappas C, Pitts D, Avery R, Pavlakis M, Del Busto R, DeNofrio D, Blumberg E A, Schoenfeld D A, Donohue T, Fisher S A, Fishman J A
机构信息
Infectious Disease Unit, Massachusetts General Hospital, Boston, Massachusetts 02114-2696, USA.
出版信息
Transpl Infect Dis. 2000 Sep;2(3):112-7.
BACKGROUND
Optimal prophylaxis against cytomegalovirus (CMV) disease for organ transplant patients at risk for primary infection (donor seropositive, recipient seronegative, D+R-) remains to be determined. We hypothesized that prolonged oral ganciclovir therapy following intravenous therapy would provide increased protection.
METHODS
A total of 155 evaluable D+R- organ transplant recipients from 13 transplant centers were entered into the study: all received intravenous ganciclovir (5 mg/kg/day) for 5-10 days and then either oral acyclovir (400 mg tid) or oral ganciclovir (1 g tid) for an additional 12 weeks. Patients were assigned to their treatment groups at a central randomization site, with a separate randomization scheme for each of the organs transplanted (kidney, heart, or liver). In the case of kidney transplants, the patients were stratified according to source of the kidney (living related vs. cadaveric donor). The primary endpoint was the incidence of CMV disease in the first six months post-transplant.
RESULTS
Treatment with oral ganciclovir was associated with a significant decrease in the incidence of symptomatic disease or viremia when compared with the oral acyclovir group (32% vs. 50%, P<0.05). This difference was most marked in terms of tissue invasive disease: only 3 of 15 symptomatic patients in the ganciclovir group vs. 10 of 21 in the acyclovir group developed tissue-invasive infection (P<0.05). There was a significant difference in the time to CMV disease or viremia in the two groups: mean time 212+/-17 days post-transplant for the acyclovir group vs. 291+/-13 days for the ganciclovir group (P<0.001). The incidence of allograft rejection was 34% in the ganciclovir group and 46% in the acyclovir group (P=NS). Leukopenia was more common in the ganciclovir group (P<0.05), but in no case did it require drug discontinuation. Ganciclovir resistance did not develop in this study.
CONCLUSION
Prophylaxis with oral ganciclovir following a brief course of intravenous ganciclovir provides useful protection against primary CMV disease.
背景
对于有原发性感染风险的器官移植患者(供体血清学阳性,受体血清学阴性,D+R-),针对巨细胞病毒(CMV)疾病的最佳预防措施仍有待确定。我们假设静脉治疗后延长口服更昔洛韦治疗将提供更大的保护。
方法
来自13个移植中心的总共155名可评估的D+R-器官移植受者进入该研究:所有人接受静脉注射更昔洛韦(5mg/kg/天)5-10天,然后接受口服阿昔洛韦(400mg每日三次)或口服更昔洛韦(1g每日三次)额外12周。患者在一个中央随机化地点被分配到他们的治疗组,针对每种移植器官(肾脏、心脏或肝脏)有单独的随机化方案。对于肾移植,患者根据肾脏来源(亲属活体供体与尸体供体)进行分层。主要终点是移植后前六个月CMV疾病的发生率。
结果
与口服阿昔洛韦组相比,口服更昔洛韦治疗与有症状疾病或病毒血症的发生率显著降低相关(32%对50%,P<0.05)。这种差异在组织侵袭性疾病方面最为明显:更昔洛韦组15名有症状患者中只有3名发生组织侵袭性感染,而阿昔洛韦组21名中有10名发生(P<0.05)。两组在发生CMV疾病或病毒血症的时间上有显著差异:阿昔洛韦组移植后平均时间为212±17天,而更昔洛韦组为291±13天(P<0.001)。更昔洛韦组同种异体移植排斥的发生率为34%,阿昔洛韦组为46%(P=无显著性差异)。白细胞减少在更昔洛韦组更常见(P<0.05),但在任何情况下都不需要停药。本研究中未出现更昔洛韦耐药。
结论
在短期静脉注射更昔洛韦后进行口服更昔洛韦预防可有效预防原发性CMV疾病。
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