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耐受性、抑制作用与胎儿同种异体移植物

Tolerance, suppression and the fetal allograft.

作者信息

Aluvihare Varuna R, Kallikourdis Marinos, Betz Alexander G

机构信息

Laboratory of Molecular Biology, Medical Research Council, University of Cambridge, Hills Road, Cambridge, CB2 2QH, UK.

出版信息

J Mol Med (Berl). 2005 Feb;83(2):88-96. doi: 10.1007/s00109-004-0608-2. Epub 2004 Dec 17.

Abstract

In solid organ transplantation the recipient immune system recognises foreign alloantigens expressed by the graft. This results in an immune attack of the transplanted organ leading to rejection, which can be prevented only by therapeutic immunosuppression. During pregnancy the fetus should also be rejected by the maternal immune system, since it expresses antigens derived from the father. Whilst the immune system retains the ability to respond to foreign antigen, tolerance mechanisms ensure that inappropriate responses against self-antigen are prevented. Maternal immune aggression directed against the fetus is partly inhibited by peripheral tolerance mechanisms that act locally to deplete cells capable of attacking the fetus. Other local mechanisms inhibit the pathways that cause tissue damage after immune activation. Recent studies in mice and humans indicate that the maternal immune system undergoes a more systemic change that promotes materno-fetal tolerance. Naturally occurring regulatory T cells, which are commonly associated with maintaining tolerance to self-antigens, can also suppress maternal allo-responses targeted against the fetus. We review the mechanisms that mediate materno-fetal tolerance, with particular emphasis on changes in regulatory T cell function during pregnancy and discuss their implications.

摘要

在实体器官移植中,受体免疫系统会识别移植物所表达的外来同种异体抗原。这会导致对移植器官的免疫攻击,进而引发排斥反应,而这种排斥反应只有通过治疗性免疫抑制才能预防。在怀孕期间,胎儿也应被母体免疫系统排斥,因为胎儿表达来自父亲的抗原。虽然免疫系统保留了对外来抗原作出反应的能力,但耐受机制可确保防止对自身抗原的不适当反应。针对胎儿的母体免疫攻击部分受到外周耐受机制的抑制,这些机制在局部发挥作用,消耗能够攻击胎儿的细胞。其他局部机制会抑制免疫激活后导致组织损伤的途径。最近在小鼠和人类身上的研究表明,母体免疫系统会发生更全身性的变化,从而促进母胎耐受。天然存在的调节性T细胞通常与维持对自身抗原的耐受性相关,它也能抑制针对胎儿的母体同种异体反应。我们综述了介导母胎耐受的机制,特别强调怀孕期间调节性T细胞功能的变化,并讨论其意义。

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