妊娠期的调节性T细胞。

Springer seminars in immunopathology Pub Date : 2006-08-01 Epub Date: 2006-07-13 DOI:10.1007/s00281-006-0023-6
Ana Claudia Zenclussen
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引用次数: 104

摘要

耐受机制负责胎儿在母体子宫内的存活,而不会受到母体免疫系统细胞的攻击,尽管它们直接接触。调节性T细胞(Treg)被认为是对携带同种异体抗原的胎儿耐受的重要参与者。最近的证据证实,Treg数量在怀孕期间增加,最重要的是,Treg数量的减少与胎儿的免疫排斥有关。通过将正常妊娠小鼠的CD4(+)/CD25(+) Treg细胞过继转移到易流产的动物体内,可以预防这种情况。Treg防止流产,同时创造一个以高水平tgf - β、LIF和HO-1为特征的短暂耐受性微环境。Treg水平下调在人类流产期间也有报道。此外,我们有证据表明,为了起到保护作用,Treg需要在怀孕期间被男性抗原激活。
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Regulatory T cells in pregnancy.

Tolerance mechanisms are responsible for the survival of the fetus within the maternal uterus without being attacked by the cells of the maternal immune system despite their direct contact. Regulatory T cells (Treg) were claimed to be important players in the tolerance towards the fetus bearing alloantigens. Recent evidence confirmed an augmentation in the number of Treg during pregnancy and, most importantly, diminished numbers of Treg were associated with immunological rejection of the fetus. This could be prevented by adoptively transferring CD4(+)/CD25(+) Treg cells from normal pregnant mice into abortion-prone animals. Treg prevented abortion while creating a transient tolerant microenvironment characterized by high levels of TGF-beta, LIF, and HO-1. Downregulated levels of Treg were accordingly also reported during human miscarriage. Furthermore, we have evidence suggesting that, to be protective, Treg need to be activated by male antigens during pregnancy.

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