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输血导致的次要组织相容性抗原引起的骨髓移植排斥反应。

Transfusion-induced bone marrow transplant rejection due to minor histocompatibility antigens.

机构信息

Department of Hematology and Medical Oncology, Emory University School of Medicine, Atlanta, GA, USA.

出版信息

Transfus Med Rev. 2013 Oct;27(4):241-8. doi: 10.1016/j.tmrv.2013.08.002. Epub 2013 Oct 3.

Abstract

Traditionally, alloimmunization to transfused blood products has focused exclusively on recipient antibodies recognizing donor alloantigens present on the cell surface. Accordingly, the immunologic sequelae of alloimmunization have been antibody mediated effects (ie, hemolytic transfusion reactions, platelet refractoriness, anti-HLA and anti-HNA effects, etc). However, in addition to the above sequelae, there is also a correlation between the number of antecedent transfusions in humans and the rate of bone marrow transplant (BMT) rejection-under reduced intensity conditioning with HLA-matched or HLA-identical marrow. Bone marrow transplant of this nature is the only existing cure for a series of nonmalignant hematologic diseases (eg, sickle cell disease, thalassemias, etc); however, rejection remains a clinical problem. It has been hypothesized that transfusion induces subsequent BMT rejection through immunization. Studies in animal models have observed the same effect and have demonstrated that transfusion-induced BMT rejection can occur in response to alloimmunization. However, unlike traditional antibody responses, sensitization in this case results in cellular immune effects, involving populations such as T cell or natural killer cells. In this case, rejection occurs in the absence of alloantibodies and would not be detected by existing immune-hematologic methods. We review human and animal studies in light of the hypothesis that, for distinct clinical populations, enhanced rejection of BMT may be an unappreciated adverse consequence of transfusion, which current blood bank methodologies are unable to detect.

摘要

传统上,对输注血液制品的同种异体免疫仅专注于受体抗体识别供体同种异体抗原在细胞表面上的存在。因此,同种异体免疫的免疫后果是抗体介导的效应(即溶血性输血反应、血小板反应性降低、抗 HLA 和抗 HNA 效应等)。然而,除了上述后果外,人类输注前的次数与骨髓移植 (BMT) 排斥率之间也存在相关性——在 HLA 匹配或 HLA 相同的骨髓中进行低强度调理。这种性质的骨髓移植是一系列非恶性血液疾病(例如镰状细胞病、地中海贫血等)的唯一现有治疗方法;然而,排斥仍然是一个临床问题。人们假设输血通过免疫诱导随后的 BMT 排斥。动物模型的研究观察到了相同的效果,并表明输血诱导的 BMT 排斥可能是对同种异体免疫的反应。然而,与传统的抗体反应不同,在这种情况下致敏导致细胞免疫效应,涉及 T 细胞或自然杀伤细胞等群体。在这种情况下,排斥发生在没有同种抗体的情况下,并且不会被现有的免疫血液学方法检测到。根据假设,我们综述了人类和动物的研究,即对于不同的临床人群,BMT 的增强排斥可能是输血未被认识到的不良后果,而当前的血库方法无法检测到这种后果。

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