Ramsey G
Central Blood Bank, Pittsburgh, Pennsylvania.
Transfusion. 1991 Jan;31(1):76-86. doi: 10.1046/j.1537-2995.1991.31191096190.x.
RBC antibodies arising from transplanted organs and directed against recipient RBCs represent a well-established immunohematologic complication of solid organ transplantation. In ABO-unmatched organs, the frequency and severity of graft antibodies and hemolysis generally increase with the size (lymphoid content) of the organ, from kidney to liver to heart-lung transplants. In the cases reviewed here, the frequency of hemolysis increased in cyclosporine-treated kidney transplant recipients and O-to-A liver transplant recipients and decreased in group AB liver transplant recipients and kidney transplant recipients receiving azathioprine or low-dose postoperative graft irradiation. Available data cannot otherwise distinguish which cyclosporine-treated recipients of ABO-unmatched kidneys and livers (30-40% of total) will develop graft antibody. There has been no conclusive effect to date of the age, race, or gender of the donor or the recipient, of cadaver versus living kidney donors, or of patients' A2 or secretor status. In a few cases of living-donor kidney grafts, the donor was the patient's mother or wife who had been exposed to the recipient's RBC antigens via pregnancy. The ABO antibodies are typically IgG, appear 7 to 10 days after transplantation, and last for about a month. If immediate-spin crossmatching is done routinely, DATs are recommended in compatibility testing after ABO-unmatched transplants. Changes in the immunosuppressive regimen, such as a change from cyclosporine therapy, have not affected the duration of these antibodies. Most patients require only transfusions for this self-limited process, but six cases of hemolysis-induced acute renal failure have been reported, and one death was attributed to complications of hemolysis. RBC or plasma exchange has been performed in a few fulminant cases. RBCs of the donor's blood type are given when antibody appears. Some workers recommend such transfusion as prophylaxis at the time of surgery, although in liver transplants, the plasma accompanying a large amount of group O RBCs given perioperatively might be problematic. In several other centers, ABO-unmatched liver transplants have equivalent overall graft survivals, but the Pittsburgh adult patients with hemolysis have had reduced early graft survival. In the cases reviewed here, nine IgG Rh antibodies from kidney grafts directed against recipient RBCs have been observed, usually beginning 2 to 3 weeks after a cyclosporine-treated transplant, lasting for 2 to 6 months after operation, and causing mild hemolysis. One case represented a primary immune response from a previously unsensitized donor.(ABSTRACT TRUNCATED AT 400 WORDS)
由移植器官产生并针对受者红细胞的红细胞抗体是实体器官移植中一种公认的免疫血液学并发症。在ABO血型不匹配的器官移植中,移植抗体和溶血的频率及严重程度通常随着器官大小(淋巴组织含量)的增加而升高,从肾脏移植到肝脏移植再到心肺移植。在本文回顾的病例中,接受环孢素治疗的肾移植受者和O型到A型肝移植受者溶血频率增加,而AB型肝移植受者以及接受硫唑嘌呤或术后低剂量移植照射的肾移植受者溶血频率降低。现有数据无法区分哪些接受环孢素治疗且ABO血型不匹配的肾脏和肝脏移植受者(占总数的30% - 40%)会产生移植抗体。迄今为止,供者或受者的年龄、种族、性别、尸体供肾与活体供肾,以及患者的A2或分泌型状态均未产生确切影响。在少数活体供肾移植病例中,供者是患者的母亲或妻子,她们在孕期接触过受者的红细胞抗原。ABO抗体通常为IgG,在移植后7至10天出现,持续约一个月。如果常规进行即刻离心交叉配血,对于ABO血型不匹配移植后的相容性检测,建议进行直接抗人球蛋白试验(DAT)。免疫抑制方案的改变,如从环孢素治疗转变,并未影响这些抗体的持续时间。大多数患者在这个自限性过程中仅需输血,但已有6例溶血诱导的急性肾衰竭病例报告,1例死亡归因于溶血并发症。在少数暴发性病例中进行了红细胞或血浆置换。当出现抗体时,输注供者血型的红细胞。一些工作人员建议在手术时进行此类输血作为预防措施,尽管在肝移植中,围手术期输注大量O型红细胞时所伴随的血浆可能存在问题。在其他几个中心,ABO血型不匹配的肝移植总体移植存活率相当,但匹兹堡有溶血的成年患者早期移植存活率降低。在本文回顾的病例中,观察到9例来自肾移植的针对受者红细胞的IgG Rh抗体,通常在接受环孢素治疗的移植后2至3周开始出现,术后持续2至6个月,并导致轻度溶血。1例代表来自先前未致敏供者的初次免疫反应。(摘要截取自400字)
