首页> 外文期刊>Reproduction: The official journal of the Society for the Study of Fertility >Comparative studies of placentation and immunology in non-human primates suggest a scenario for the evolution of deep trophoblast invasion and an explanation for human pregnancy disorders
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Comparative studies of placentation and immunology in non-human primates suggest a scenario for the evolution of deep trophoblast invasion and an explanation for human pregnancy disorders

机译:比较非人类灵长类动物的胎盘免疫和免疫学研究,提出了滋养层深层浸润演变的一种情况以及人类妊娠疾病的解释

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Deep trophoblast invasion in the placental bed has been considered the hallmark of human pregnancy. It occurs by two routes, interstitial and endovascular, and results in transformation of the walls of the spiral arteries as they traverse the decidua and the inner third of the myometrium. Disturbances in this process are associated with reproductive disorders such preeclampsia. In contrast, trophoblast invasion in Old World monkeys occurs only by the endovascular route and seldom reaches the myometrium. Recently, it was shown that this pattern is maintained in gibbons, but that the human arrangement also occurs in chimpanzee and gorilla. There is an interesting parallel with results from placental immunology regarding the evolution of the major histocompatability complex class I antigen HLA-C and its cognate receptors. HLA-C is not present in Old World monkeys or gibbons. It emerged in the orangutan and became polymorphic in the lineage leading to gorilla, bonobo, chimpanzee, and human. Interaction between HLA-C1 and HLA-C2 on the surface of trophoblast and killer immunoglobulin-like receptors (KIRs) expressed by uterine natural killer cells are important regulators of trophoblast invasion. Evolution of this system in great apes may have been one prerequisite for deep trophoblast invasion but seems to have come at a price. The evidence now suggests that certain combinations of maternal genotype for KIRs and fetal genotype for HLA-C imply an increased risk of preeclampsia, fetal growth restriction, and recurrent abortion. The fetal genotype is in part derived from the father providing an explanation for the paternal contribution to reproductive disorders.
机译:胎盘床上的滋养细胞深层浸润被认为是人类怀孕的标志。它通过间质和血管内两种途径发生,并导致螺旋动脉壁横穿蜕膜和肌层内侧三分之一时发生转化。在这个过程中的干扰与生殖疾病如先兆子痫有关。相反,旧大陆猴子的滋养细胞入侵仅通过血管内途径发生,很少到达子宫肌层。最近,显示出长臂猿中保持了这种模式,但是人类的排列也发生在黑猩猩和大猩猩中。关于主要组织相容性复合体I类抗原HLA-C及其同源受体的进化,与胎盘免疫学结果令人感兴趣。 HLA-C在旧世界的猴子或长臂猿中不存在。它出现在猩猩中,并在导致大猩猩,bo黑猩猩,黑猩猩和人类的血统中变成多态。滋养细胞表面的HLA-C1和HLA-C2与子宫自然杀伤细胞表达的杀伤性免疫球蛋白样受体(KIR)之间的相互作用是滋养层细胞入侵的重要调节剂。该系统在大猿类中的进化可能已经成为滋养层细胞深层侵袭的先决条件,但似乎付出了代价。现在的证据表明,KIR的母亲基因型和HLA-C的胎儿基因型的某些组合意味着先兆子痫,胎儿生长受限和反复流产的风险增加。胎儿基因型部分来源于父亲,为父亲对生殖疾病的贡献提供了解释。

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