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在高度致敏的肾移植受者中,通过移植前免疫吸附疗法去除淋巴细胞毒性抗体。

Removal of lymphocytotoxic antibodies by pretransplant immunoadsorption therapy in highly sensitized renal transplant recipients.

作者信息

Kupin W L, Venkat K K, Hayashi H, Mozes M F, Oh H K, Watt R

机构信息

Department of Pathology, Henry Ford Hospital, Detroit, Michigan 48202.

出版信息

Transplantation. 1991 Feb;51(2):324-9. doi: 10.1097/00007890-199102000-00010.

Abstract

A high level of panel-reactive antibodies (PRA) in potential renal transplant recipients is associated with a long waiting time until transplantation and correlates inversely with graft outcome. We report our experience with the employment of immunoadsorption (IA) using a column composed to sepharose-bound staphylococcal protein A (which has a relatively selective affinity for binding IgG compared with other immunoglobulins) to decrease the PRA levels and expedite transplantation in 6 highly sensitized potential renal transplant recipients (1 primary and 5 awaiting second transplants). All patients had PRA levels of greater than or equal to 70% for a duration of 1 year prior to IA. Only patients with antibody specificity localized to 1 or 2 HLA A or B antigens were accepted for the study. IA procedures were performed on alternate days until a twofold decrease in antibody titer had occurred (maximum: 6 procedures). Repeat procedures were initiated if the HLA antibody titer returned to its baseline value. Intravenous cyclophosphamide (CY) (10 mg/kg/day every 3 weeks) and methylprednisolone (MP) (0.5 mg/kg/day) were provided as adjunctive immunosuppression until transplantation. A total of 44 immunoadsorption procedures were performed (27 primary and 17 repeat) with treatment of 2.49 +/- 0.02 plasma volumes per session. Serum IgG concentration decreased 95 +/- 3% and PRA activity decreased 75 +/- 16% after the primary treatment course. Four patients received cadaveric grafts within 3.7 +/- 1.2 months following the last IA procedure. Three grafts are functioning at 1 year, 8 months, and 8 weeks posttransplant. The remaining graft demonstrated primary nonfunction. All four patients had a past positive crossmatch using pre-IA sera with their respective donors. Patients not transplanted exhibited rapid resynthesis of IgG and a return of the PRA towards baseline levels within a few weeks after IA. We conclude that IA can effectively remove HLA antibodies and expedite graft availability in highly sensitized patients.

摘要

潜在肾移植受者体内高水平的群体反应性抗体(PRA)与移植前漫长的等待时间相关,且与移植结果呈负相关。我们报告了对6例高度致敏的潜在肾移植受者(1例初次等待移植,5例等待二次移植)采用免疫吸附(IA)的经验,该方法使用由琼脂糖结合葡萄球菌蛋白A组成的柱体(与其他免疫球蛋白相比,其对IgG的结合具有相对选择性亲和力)来降低PRA水平并加快移植进程。在进行IA之前,所有患者PRA水平持续1年大于或等于70%。仅抗体特异性定位于1种或2种HLA A或B抗原的患者被纳入研究。IA程序每隔一天进行一次,直至抗体滴度下降两倍(最多6次程序)。如果HLA抗体滴度恢复到基线值,则启动重复程序。在移植前,静脉注射环磷酰胺(CY)(每3周10mg/kg/天)和甲泼尼龙(MP)(0.5mg/kg/天)作为辅助免疫抑制治疗。共进行了44次免疫吸附程序(27次初次和17次重复),每次治疗2.49±0.02个血浆容量。初次治疗疗程后,血清IgG浓度下降95±3%,PRA活性下降75±16%。4例患者在最后一次IA程序后3.7±1.2个月内接受了尸体肾移植。3例移植肾在移植后1年、8个月和8周时功能良好。其余移植肾表现为原发性无功能。所有4例患者在IA前血清与各自供者的交叉配型均为阳性。未接受移植的患者在IA后几周内IgG迅速重新合成,PRA恢复至基线水平。我们得出结论,IA可有效清除HLA抗体并加快高度致敏患者的移植肾获取。

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