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本文引用的文献

1
Studies on orthotopic homotransplantation of the canine heart.犬心脏原位同种移植的研究。
Surg Forum. 1960;11:18-9.
2
Infections after liver transplantation. An analysis of 101 consecutive cases.肝移植术后感染。101例连续病例分析。
Medicine (Baltimore). 1988 Mar;67(2):132-43. doi: 10.1097/00005792-198803000-00006.
3
Lessons learned in pediatric heart transplantation.
Ann Thorac Surg. 1989 Nov;48(5):617-22; discussion 622-3. doi: 10.1016/0003-4975(89)90774-1.
4
Infections in pediatric orthotopic heart transplant recipients.小儿原位心脏移植受者的感染
Pediatr Infect Dis J. 1989 Feb;8(2):87-93.
5
A highly sensitive method to assay FK-506 levels in plasma.一种检测血浆中FK-506水平的高灵敏度方法。
Transplant Proc. 1987 Oct;19(5 Suppl 6):23-9.
6
A working formulation for the standardization of nomenclature in the diagnosis of heart and lung rejection: Heart Rejection Study Group. The International Society for Heart Transplantation.心脏和肺排斥反应诊断命名标准化的工作方案:心脏排斥反应研究组。国际心脏移植学会。
J Heart Transplant. 1990 Nov-Dec;9(6):587-93.
7
Posttransplant lymphoproliferative disease in thoracic organ transplant patients: ten years of cyclosporine-based immunosuppression.胸器官移植患者的移植后淋巴细胞增生性疾病:基于环孢素的免疫抑制治疗十年
J Heart Lung Transplant. 1991 Nov-Dec;10(6):877-86; discussion 886-7.
8
Primary cardiac angiosarcoma: a clinicopathologic study of six cases.原发性心脏血管肉瘤:6例临床病理研究
J Thorac Cardiovasc Surg. 1992 Apr;103(4):655-64.
9
Clinical trial of FK 506 immunosuppression in adult cardiac transplantation.FK506免疫抑制在成人心脏移植中的临床试验。
Ann Thorac Surg. 1992 Aug;54(2):205-10; discussion 210-1. doi: 10.1016/0003-4975(92)91371-f.

十年(1982年至1992年)小儿心脏移植及FK 506免疫抑制的影响

A decade (1982 to 1992) of pediatric cardiac transplantation and the impact of FK 506 immunosuppression.

作者信息

Armitage J M, Fricker F J, del Nido P, Starzl T E, Hardesty R L, Griffith B P

机构信息

Department of Surgery, University of Pittsburgh School of Medicine, PA.

出版信息

J Thorac Cardiovasc Surg. 1993 Mar;105(3):464-72; discussion 472-3.

PMID:7680396
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2948867/
Abstract

The decade from 1982 through 1992 witnessed tremendous growth in pediatric cardiac transplantation. At Children's Hospital of Pittsburgh 66 cardiac transplants were performed during this period (age range 7 hours to 18 years). The cause of cardiomyopathy was congenital (n = 30), cardiomyopathy (n = 29), myocarditis (n = 2), doxorubicin toxicity (n = 2), ischemic (n = 1), valvular (n = 1), and cardiac angiosarcoma (n = 1). Nine children (14%) required mechanical circulatory support before transplantation: extracorporeal membrane oxygenation (n = 8) and Novacor left ventricular assist system (n = 1) (Baxter Healthcare Corp., Novacor Div., Oakland, Calif.). The mean follow-up time was 2 years (range 4 months to 8 years). The overall survival in the group was 67%. In children with congenital heart disease (> 6 months of age) the perioperative (30 day) mortality was 66% before mid-1988 (n = 10) and 0% since mid-1988 (n = 11). The late mortality (> 30 days) in children with cardiomyopathy transplanted prior to mid-1988 was 66% (n = 14) and 7% since mid-1988 (n = 15). Since mid-1988 1- and 3-year survival was 82% in children with congenital heart disease and 90% in children with cardiomyopathy. Twenty-six children have had FK 506 as their primary immunosuppressive therapy since November 1989. Survival in this group was 82% at 1 and 3 years. The actuarial freedom from grade 3A rejection in the FK group was 60% at 3 and 6 months after transplantation versus 20% and 12%, respectively, in the 15 children operated on before the advent of FK 506, who were treated with cyclosporine-based triple-drug therapy (p < 0.001, Mantel-Cox and Breslow). Twenty of 24 children (83%) in the FK 506 group are receiving no steroids. The prevalence of posttransplantation hypertension was 4% in the FK 506 group versus 70% in the cyclosporine group (p < 0.001, Fisher). Renal toxicity in children treated with FK 506 has been mild. Additionally, eight children have been switched to FK 506 because of refractory rejection and drug toxicity. FK 506 has not produced hirsutism, gingival hyperplasia, or abnormal facial bone growth. The absence of these debilitating side effects, together with the observed immune advantage and steroid-sparing effects of FK 506, hold tremendous promise for the young patient facing cardiac transplantation and a future wedded to immunosuppression.

摘要

从1982年到1992年的这十年间,小儿心脏移植手术取得了巨大的发展。在匹兹堡儿童医院,这期间共进行了66例心脏移植手术(年龄范围从7小时至18岁)。心肌病的病因包括先天性(n = 30)、心肌病(n = 29)、心肌炎(n = 2)、阿霉素毒性(n = 2)、缺血性(n = 1)、瓣膜性(n = 1)以及心脏血管肉瘤(n = 1)。9名儿童(14%)在移植前需要机械循环支持:体外膜肺氧合(n = 8)和诺瓦科尔左心室辅助系统(n = 1)(百特医疗保健公司,诺瓦科尔分部,加利福尼亚州奥克兰)。平均随访时间为2年(范围4个月至8年)。该组的总体生存率为67%。在先天性心脏病患儿(>6个月龄)中,1988年年中之前围手术期(30天)死亡率为66%(n = 10),自1988年年中以来为0%(n = 11)。1988年年中之前接受移植的心肌病患儿晚期死亡率(>30天)为66%(n = 14),自1988年年中以来为7%(n = 15)。自1988年年中以来,先天性心脏病患儿1年和3年生存率为82%,心肌病患儿为90%。自1989年11月以来,26名儿童将FK 506作为主要免疫抑制疗法。该组1年和3年生存率为82%。FK组移植后3个月和6个月时3A级排斥反应的无事件生存率分别为60%,而在FK 506出现之前接受手术、采用基于环孢素的三联药物疗法治疗的15名儿童中,这一比例分别为20%和12%(p < 0.001,Mantel - Cox和Breslow检验)。FK 506组24名儿童中有20名(83%)未接受类固醇治疗。FK 506组移植后高血压患病率为4%,而环孢素组为70%(p < 0.001,Fisher检验)。接受FK 506治疗的儿童肾毒性较轻。此外,8名儿童因难治性排斥反应和药物毒性转而接受FK 506治疗。FK 506未导致多毛症、牙龈增生或面部骨骼异常生长。这些令人衰弱的副作用的缺失,以及所观察到的FK 506的免疫优势和类固醇节省效应,为面临心脏移植且未来离不开免疫抑制治疗的年轻患者带来了巨大的希望。