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低强度免疫抑制下心脏移植后严重感染发生率降低。

Reduced incidence of severe infection after heart transplantation with low-intensity immunosuppression.

作者信息

Reid K R, Menkis A H, Novick R J, Pflugfelder P W, Kostuk W J, Reid J, Whitby J L, Powell A M, McKenzie F N

机构信息

University Hospital, London, Ontario, Canada.

出版信息

J Heart Lung Transplant. 1991 Nov-Dec;10(6):894-900.

PMID:1756154
Abstract

Despite advances in immunosuppressive therapy and prolonged graft and patient survival, infection after heart transplantation remains problematic. From January 1987 through June 1989, 104 heart transplantations were performed in 100 patients. Immunosuppression induction was by antilymphocyte globulin for 7 days, with oral cyclosporine introduced on stabilization of kidney function (day 3). Steroid therapy was rapidly tapered, and azathioprine was added only in cases of positive donor crossmatch or steroid-resistant rejection. No reverse isolation was used. Twenty-two deaths occurred, one from sepsis. Actuarial survival at 6 months, at 1 year, and at 2 years was 85% +/- 4%, 81% +/- 3%, and 75% +/- 4%, respectively. Fifty-four patients had 81 infections, of which 21 were bacterial; 83% of these episodes were treated. Sixty infections were opportunistic (85% viral), and only 23% necessitated treatment. Actuarial infection-free rates (all types necessitating treatment) at 1 month, at 6 months, and at 2 years were 83% +/- 4%, 75% +/- 5%, and 75% +/- 5%, respectively. Of the 100 transplant recipients, 66% were treated with azathioprine; 47 patients (69%) had an infection, whereas only seven (19%) of the patients not receiving azathioprine became infected (p less than 0.00001). Rejection was noted in 66% of patients, with a median time to the first episode of 4 weeks. A low-intensity immunosuppressive regimen has resulted in fewer serious infections, with acceptable graft loss from rejection. Increased infection surveillance is required for the first 30 days postoperatively and after treatment of rejection episodes.

摘要

尽管免疫抑制疗法取得了进展,移植心脏和患者的存活时间得以延长,但心脏移植后的感染问题仍然存在。从1987年1月至1989年6月,100例患者接受了104例心脏移植手术。免疫抑制诱导采用抗淋巴细胞球蛋白治疗7天,待肾功能稳定(第3天)后开始口服环孢素。类固醇疗法迅速减量,仅在供体交叉配型阳性或类固醇抵抗性排斥反应的病例中添加硫唑嘌呤。未采用反向隔离措施。22例患者死亡,其中1例死于败血症。6个月、1年和2年的精算生存率分别为85%±4%、81%±3%和75%±4%。54例患者发生了81次感染,其中21次为细菌感染;这些感染事件的83%得到了治疗。60次感染为机会性感染(85%为病毒感染),仅23%需要治疗。1个月、6个月和2年的精算无感染率(所有需要治疗的类型)分别为83%±4%、75%±5%和75%±5%。100例移植受者中,66%接受了硫唑嘌呤治疗;47例患者(69%)发生了感染,而未接受硫唑嘌呤治疗的患者中只有7例(19%)发生了感染(p<0.00001)。66%的患者出现了排斥反应,首次发作的中位时间为4周。低强度免疫抑制方案导致严重感染减少,排斥反应造成的移植心脏丢失可接受。术后前30天以及排斥反应发作治疗后需要加强感染监测。

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