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妊娠后半期小鼠子宫、胚胎及胎盘中免疫球蛋白的定位

Localization of immunoglobulins in the mouse uterus, embryo, and placenta during the second half of pregnancy.

作者信息

Parr E L, Parr M B

出版信息

J Reprod Immunol. 1985 Nov;8(2-3):153-71. doi: 10.1016/0165-0378(85)90038-5.

Abstract

Throughout the second half of pregnancy in mice there were many plasma cells containing immunoglobulins A (IgA) and G (IgG) in the uterine endometrium. There was intense staining of IgA in uterine glands at all stages, but little staining of IgG. The staining of both immunoglobulins (Igs) in the luminal epithelium was moderate to dark on day 11, slight on day 14, and increased from day 16 to term. From day 14 to term the endometrium exhibited folds or villi around each placenta. The cores of the villi contained many plasma cells of both isotypes, and the staining of extracellular Igs in the villous cores was darker than in nonvillous endometrium. Both Igs were detected in the uterine lumen, and in visceral and parietal yolk sac endoderm cells at all stages. Near term, the staining of Igs in the visceral yolk sac was darkest in the peripheral villous portion adjacent to the endometrial villi. From day 14 to term IgG was present in the visceral yolk sac mesenchyme and embryo, consistent with its transfer from the uterine lumen to the embryo via the vitelline circulation. In contrast, IgA was not detected in yolk sac mesenchyme until day 19, when only slight staining was observed, and IgA was never detected in the embryo. Most trophoblast giant cells contained both Igs on day 11. During the remainder of pregnancy, there was staining of both Igs in labyrinthine trophoblast and in a few giant cells adjacent to the parietal yolk sac on the placenta, but there was negligible staining in the spongiotrophoblast region. Our observations suggest that the local immune system in the mouse uterus may protect the embryo during the second half of pregnancy by secreting anti-microbial immunoglobulins A and G into the uterine lumen surrounding the visceral yolk sac, and may at the same time contribute to the transfer of maternal IgG to the embryo via the yolk sac and vitelline circulation.

摘要

在小鼠妊娠后半期,子宫子宫内膜中有许多含有免疫球蛋白A(IgA)和G(IgG)的浆细胞。在所有阶段,子宫腺中IgA染色强烈,但IgG染色很少。腔上皮中两种免疫球蛋白(Igs)的染色在第11天为中度至深色,第14天为浅色,从第16天到足月增加。从第14天到足月,子宫内膜在每个胎盘周围呈现褶皱或绒毛。绒毛核心含有许多两种同种型的浆细胞,绒毛核心中细胞外Igs的染色比非绒毛子宫内膜中的更深。在所有阶段,两种Igs都在子宫腔、内脏和壁层卵黄囊内胚层细胞中被检测到。接近足月时,内脏卵黄囊中Igs的染色在与子宫内膜绒毛相邻的外周绒毛部分最深。从第14天到足月,IgG存在于内脏卵黄囊间充质和胚胎中,这与其通过卵黄循环从子宫腔转移到胚胎一致。相比之下,直到第19天才在卵黄囊间充质中检测到IgA,当时仅观察到轻微染色,并且在胚胎中从未检测到IgA。大多数滋养层巨细胞在第11天含有两种Igs。在妊娠剩余时间里,迷路滋养层和胎盘上与壁层卵黄囊相邻的一些巨细胞中有两种Igs的染色,但海绵滋养层区域的染色可忽略不计。我们的观察结果表明,小鼠子宫中的局部免疫系统可能在妊娠后半期通过向包围内脏卵黄囊的子宫腔中分泌抗菌免疫球蛋白A和G来保护胚胎,并且可能同时通过卵黄囊和卵黄循环促进母体IgG向胚胎的转移。

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