[HLA-G:从胎母耐受到器官移植]。

E D Carosella
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摘要

卡罗塞拉(E.D. Carosella)是证明HLA-G分子对滋养细胞起保护作用的先驱,滋养细胞形成屏障,保护胎儿免受母亲的免疫反应和随后的排斥。这种非经典HLA I类分子首先在受精卵细胞上表达,从而使子宫着床成为可能,然后在缺乏经典I类和II类抗原的胎盘滋养细胞表面表达。他首次在体外证明了存在于胎儿细胞滋养层细胞表面的HLA-G分子对母体子宫蜕膜NK细胞进行溶解的保护作用,无论是半同种异体组合(母体子宫NK细胞和它们自己的胎儿细胞滋养层细胞)还是同种异体组合(来自不同胎儿的不同母体子宫NK细胞和细胞滋养层细胞)。这种蛋白质的阻断会对胎儿细胞产生重要的细胞毒性。此外,他还发现HLA-G分子可以作为t淋巴细胞、NK细胞和抗原呈递细胞(APC)的抑制剂。通过他的发现,Carosella也首次展示了三个主要的临床后果:1)HLA-G分子是至关重要的,因为这些分子的表达改变会导致流产和妊娠失败,即复发性自然流产和子痫前期疾病。胚胎中可溶性HLA-G分子的表达是胚胎着床的必要前提。II)在同种异体移植(心脏、肾脏和肝肾移植)中,HLA-G蛋白的表达可显著减少急性排斥反应,并无慢性排斥反应。III)最后,这种在恶性细胞上的表达对抗肿瘤反应有负面的功能影响。因此,HLA-G分子的表达构成了一种逃避免疫监视的机制,就像胎儿细胞保护自己免受母体免疫细胞的攻击一样。
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[HLA-G: from feto-maternal tolerance to organ grafting].

E.D. Carosella was the pioneer who demonstrated the protective role of the HLA-G molecule on trophoblasts, which form a shield protecting the fetus from the immune reaction of its mother and subsequent reject. This non-classical HLA class I molecule is first expressed on the fertilized ovocyte, thus enabling a uterine implantation and then on the surface of the placenta trophoblast where the classical class I and II antigens are absent. He brought the first demonstration ex vivo of the protector role of HLA-G molecule present on the surface of fetal cytotrophoblast cells versus the lysis carried out by maternal decidual uterine NK cells, in both semi-allogenic combinations (maternal uterine NK cells and their own fetal cytotropohoblast counterparts) and allogenic combinations (different maternal uterine NK cells and cytotrophoblasts from different fetuses). The blockage of this protein triggers off an important cytotoxicity towards the fetal cells. Furthermore, he showed that HLA-G molecules act as an inhibitor of the T-lymphocytes, NK cells and antigen presenting cells (APC). Through his discovery Carosella also shows for the first time the three major clinical consequences: I) HLA-G molecules are crucial, as an altered expression of these molecules would lead to abortion and failed pregnancies, i.e. recurrent spontaneous abortions and preeclamptic disease. The embryo expression of soluble HLA-G molecules is a mandatory prerequisite to implantation. II) In allogenic transplantation (heart, kidney and liver-kidney graft) the expression of HLA-G protein significantly reduces acute rejection and showed an absence of chronic rejections. III) Finally, this expression on the malignant cells has a negative functional impact in the anti-tumour response. So the expression of HLA-G molecule constitutes an escape mechanism from immunosurveillance, just as the fetal cells protect themselves from the aggression of maternal immune cells.

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