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进行基因检测以确定实体器官移植中溶血性抗体的来源。

Genetic testing to resolve the source of haemolytic antibody in solid organ transplantation.

机构信息

Division of Transfusion Medicine, Department of Laboratory Medicine, University of Washington School of Medicine, Seattle, WA, United States of America.

出版信息

Blood Transfus. 2019 Jul;17(4):307-311. doi: 10.2450/2019.0054-19. Epub 2019 Jun 5.

Abstract

BACKGROUND

Antibody-mediated haemolysis due to passenger lymphocyte syndrome arising in the setting of solid organ transplant can be devastating. Some degree of passenger lymphocyte syndrome is said to occur in up to 10% of ABO mismatched renal transplants, 40% of ABO mismatched liver transplants, and 70% of ABO mismatched heart-lung transplants; a reflection of the number of memory B cells transplanted with the organ. Passenger lymphocyte syndrome is less common with minor red cell antigens but can still be severe.

MATERIALS AND METHODS

We review a series of patients who developed passenger lymphocyte syndrome after solid organ transplantation. Conventional serological testing was performed using tube and solid-phase testing. Molecular testing was performed using a gene-chip array.

RESULTS

In patients receiving a minor antigen mismatched organ transplant and multiple allogenic red cell transfusions, serological methods proved insufficient to resolve the source of minor blood group antibodies that arose in the aftermath of the transplant. Genetic testing was able to clearly resolve donor and recipient types.

DISCUSSION

Passenger lymphocyte syndrome after mismatched organ transplantation is not rare, but the syndrome associated with non-ABO antibodies occurs in a much smaller subset of these cases. The mixtures of organ donor, recipient, and other transfused red blood cells profoundly limit the usefulness of serological testing. Genetic assignment of minor blood types to donor and recipient can guide therapy and inform prognosis.

摘要

背景

在实体器官移植背景下,由于过客淋巴细胞综合征引起的抗体介导的溶血可能是毁灭性的。据说在多达 10%的 ABO 不相容肾移植、40%的 ABO 不相容肝移植和 70%的 ABO 不相容心肺移植中会发生一定程度的过客淋巴细胞综合征;这反映了与器官一起移植的记忆 B 细胞的数量。过客淋巴细胞综合征在次要红细胞抗原中较少见,但仍可能很严重。

材料和方法

我们回顾了一系列在实体器官移植后发生过客淋巴细胞综合征的患者。使用试管和固相检测进行常规血清学检测。使用基因芯片阵列进行分子检测。

结果

在接受次要抗原不相容器官移植和多次同种异体红细胞输注的患者中,血清学方法不足以确定移植后出现的次要血型抗体的来源。基因检测能够明确区分供体和受体类型。

讨论

不相容器官移植后的过客淋巴细胞综合征并不罕见,但与非 ABO 抗体相关的综合征在这些病例中的一个小得多的亚组中发生。器官供体、受体和其他输注的红细胞的混合物极大地限制了血清学检测的有用性。将次要血型的遗传分配给供体和受体可以指导治疗并告知预后。

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引用本文的文献

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