Marcos Amadeo, Eghtesad Bijan, Fung John J, Fontes Paulo, Patel Kusum, Devera Michael, Marsh Wallis, Gayowski Timothy, Demetris Anthony J, Gray Edward A, Flynn Bridget, Zeevi Adriana, Murase Noriko, Starzl Thomas E
Thomas E. Starzl Transplantation Institute, Pittsburgh, Pennsylvania, USA.
Transplantation. 2004 Oct 15;78(7):966-71. doi: 10.1097/01.tp.0000142674.78268.01.
We have proposed that the mechanisms of alloengraftment and variable acquired tolerance can be facilitated by minimum posttransplant immunosuppression. It was further suggested that the efficacy of minimalistic treatment could be enhanced by preoperative recipient conditioning with an antilymphoid antibody preparation. A total of 76 adults (38 hepatitis C virus [HCV], 38 HCV) were infused with 30 mg alemtuzumab before primary cadaveric liver transplantation and maintained afterward on daily monotherapy unless breakthrough rejection mandated additional agents. In stable patients, the intervals between tacrolimus doses were lengthened ("spaced weaning") after approximately 4 months. Eighty-four contemporaneous nonlymphoid-depleted liver recipients (58 HCV, 26 HCV) were treated with conventional postoperative immunosuppression. The overall incidence of rejection was similar with the two strategies of immunosuppression. With follow-ups of 14 to 22 months, patient and primary graft survival in HCV cases are 97% and 90%, respectively, with alemtuzumab depletion plus minimal immunosuppression versus 71% and 70%, respectively, under conventional immunosuppression. In HCV recipients, current patient and graft survival in the alemtuzumab-pretreated group are 71% and 70% versus 65% and 54%, respectively, under conventional treatment. With both strategies of immunosuppression, the adverse effect of preexisting HCV on survival parameters and graft function already was significant at the 1-year milestone, but its extent was not evident until the second year. With or without HCV, 62% of the 64 surviving lymphoid-depleted patients are on spaced immunosuppression, and four patients receive no immunosuppression. Lymphoid depletion with alemtuzumab and minimalistic maintenance immunosuppression is a practical strategy of liver transplantation in HCV recipients but not HCV recipients.
我们提出,通过最小化移植后免疫抑制可促进同种异体移植和可变获得性耐受的机制。进一步表明,术前用抗淋巴细胞抗体制剂对受体进行预处理可增强简约治疗的疗效。在初次尸体肝移植前,共76名成年人(38名丙型肝炎病毒[HCV]感染者,38名HCV感染者)输注了30mg阿仑单抗,术后维持每日单一疗法,除非出现突破性排斥反应才需要加用其他药物。在病情稳定的患者中,大约4个月后延长他克莫司给药间隔(“间隔撤药”)。84名同期未进行淋巴细胞清除的肝移植受者(58名HCV感染者,26名HCV感染者)接受了传统的术后免疫抑制治疗。两种免疫抑制策略的排斥反应总体发生率相似。随访14至22个月,HCV病例中,采用阿仑单抗清除加最小化免疫抑制治疗的患者和原发性移植物存活率分别为97%和90%,而传统免疫抑制治疗下分别为71%和70%。在HCV受体中,阿仑单抗预处理组目前的患者和移植物存活率分别为71%和7%,而传统治疗下分别为65%和54%。采用两种免疫抑制策略时,术前存在的HCV对生存参数和移植物功能的不良影响在1年里程碑时就已很显著,但直到第二年其程度才明显显现。无论有无HCV感染,64名存活的淋巴细胞清除患者中有62%采用间隔免疫抑制,4名患者未接受免疫抑制。用阿仑单抗进行淋巴细胞清除和最小化维持免疫抑制是HCV受体肝移植的一种实用策略,但不适用于非HCV受体。