Immunological and genetic factors influencing pregnancy and development.

T J Gill
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Abstract

Hypotheses concerning reproductive competence focus on immunological and genetic mechanisms. The immunological hypothesis involves arguments that an immune response is necessary for implantation (or at least increased reproductive capacity), the antibody response to the placental antigens is composed of "blocking" antibodies, immunosuppressive factors are produced during pregnancy, and HLA antigen sharing in humans having chronic spontaneous abortions (CSA) causes a decreased immune response. The most potent antigen on the placenta is a class I molecule different from the classical transplantation antigens: Pa in the rat and TLX in the human. The genetic hypothesis states that CSA may be due to the presence of major histocompatibility complex (MHC)-linked, recessive lethal genes in the fetus and that the sharing of HLA antigens is just a marker for this segment of chromosome. Recessive lethal genes linked to the MHC exist in mice and rats and possibly in humans. They could act by themselves to cause fetal loss, or they could act epistatically with nonMHC lethal genes. This type of interaction occurs in the rat between the MHC-linked grc and Tal or Hre. Recent work in our laboratory has shown that the grc also increases susceptibility to the development of cancer following the feeding of a chemical carcinogen. This unique finding presents a new and powerful approach to exploring the relationship between embryogenesis and carcinogenesis.

影响妊娠和发育的免疫和遗传因素。
关于生殖能力的假说主要集中在免疫和遗传机制上。免疫假说认为,植入(或至少增加生殖能力)需要免疫反应,对胎盘抗原的抗体反应是由“阻断”抗体组成的,免疫抑制因子在怀孕期间产生,慢性自然流产(CSA)患者的HLA抗原共享导致免疫反应降低。胎盘上最有效的抗原是一类分子,不同于经典的移植抗原:大鼠的Pa和人的TLX。遗传假说认为,CSA可能是由于胎儿存在主要组织相容性复合体(MHC)相关的隐性致死基因,而HLA抗原的共享只是这段染色体的标记。与MHC相关的隐性致死基因存在于小鼠和大鼠身上,也可能存在于人类身上。它们可以自己起作用导致胎儿丢失,或者它们可以与非mhc致命基因一起起作用。这种类型的相互作用发生在大鼠mhc连接的grc和Tal或Hre之间。我们实验室最近的工作表明,grc也增加了化学致癌物喂养后癌症发展的易感性。这一独特的发现为探索胚胎发生和癌变之间的关系提供了一种新的有力的方法。
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