Brunker Patricia A R
Department of Pathology; The Johns Hopkins Hospital; Baltimore, MD USA.
Chimerism. 2013 Oct-Dec;4(4):119-25. doi: 10.4161/chim.26912. Epub 2013 Nov 6.
Transfusion therapy is complicated by the production of alloantibodies to antigens present in the donor and lacking in the recipient through the poorly-understood but likely multi-factorial process of alloimmunization. The low prevalence of alloimmunization in transfused patients (6.1%) (1) suggests that processes central to immunologic tolerance may be operating in the vast majority of transfused patients who do not produce alloantibodies. Using RhD as a prototype, evidence is reviewed that the ability to make antibodies to red blood cell (RBC) antigens may result in part from immunologic tolerance acquired in utero. These ideas are extended to other examples of maternal microchimerism (MMc) of other non-inherited maternal antigens (NIMA). An evolutionary argument is offered that multi-generational immunity supports the hypothesis that MMc may partly explain the "non-responder" phenotype in RBC alloimmunization.
输血治疗因通过理解不充分但可能是多因素的同种免疫过程产生针对供体中存在而受体中缺乏的抗原的同种抗体而变得复杂。输血患者中同种免疫的低发生率(6.1%)(1)表明,免疫耐受的核心过程可能在绝大多数未产生同种抗体的输血患者中起作用。以RhD为原型,回顾了证据表明,产生针对红细胞(RBC)抗原的抗体的能力可能部分源于子宫内获得的免疫耐受。这些观点扩展到其他非遗传母体抗原(NIMA)的母体微嵌合体(MMc)的其他例子。提出了一个进化观点,即多代免疫支持MMc可能部分解释RBC同种免疫中“无反应者”表型的假说。
