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Alpha-2 macroglobulin controls trophoblast positioning in mouse implantation sites.

机译:Alpha-2巨球蛋白可控制滋养细胞在小鼠植入部位的定位。

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摘要

In humans, functional deficiency of alpha-2M is not known, implying alpha 2M is essential for gestational success. Mice, deficient in two members of the alpha-2 Macroglobulin (alpha 2M) family, i.e. alpha-2 macroglobulin (MAM) and murinoglobulin-1 (MUG-1) are viable, fertile and phenotypically normal, unless stressed (Am J Pathol, 155 (1999), 983). Here, we analysed implantation sites in MAM(-/-)/MUG-1(-/-)mice during pregnancy, a strong physiological stressor. Despite some post-implantation fetal loss, mean litter size was comparable to congenic C57Bl/6J (B6) mice, but MAM(-/-)/MUG-1(-/-)pups were significantly lighter and the sex ratio was skewed towards males. Implantation sites appeared histologically normal up to gestational day (gd) 8. By gd 10, extensive over-development of trophoblasts was evident, accompanied by relative deficits in decidua, in the mural mesometrial lymphoid aggregates of pregnancy and in uterine Natural Killer cells. At gd 10-12, decidual spiral arteries were dilated but abnormally cuffed by trophoblasts that extended anomalously, for midgestation, to the myometrial circular smooth muscle. Ultrastructurally, trophoblasts in the mesometrial decidua made intimate contact with endothelial cells that were shedding membrane fragments. These findings demonstrate that alpha 2M, and thereby proteinases and/or cytokines whose bio-availability is regulated by alpha 2M, exert significant decidual regulation on trophoblast invasion.
机译:在人类中,尚不知道α-2M的功能缺陷,这意味着α2M对于妊娠成功至关重要。除非存在压力,否则缺乏两个alpha-2巨球蛋白(alpha 2M)家族成员的小鼠,即alpha-2巨球蛋白(MAM)和murinoglobulin-1(MUG-1)是活的,可育的和表型正常的。 155(1999),983)。在这里,我们分析了怀孕期间MAM(-/-)/ MUG-1(-/-)小鼠的植入部位,这是一种强烈的生理应激源。尽管植入后有一些胎儿遗失,但平均产仔数与同类C57Bl / 6J(B6)小鼠相当,但MAM(-/-)/ MUG-1(-/-)幼仔明显变轻,性别比偏向男性。直到妊娠第8天,植入部位在组织学上似乎是正常的。到了第10天,可见滋养细胞大量过度发育,并伴随着蜕膜,妊娠的壁间质淋巴样聚集体和子宫自然杀伤细胞的相对缺乏。在10-12岁时,蜕膜螺旋动脉扩张,但被滋养细胞异常地套上,滋养细胞在妊娠中期异常延伸至肌层环形平滑肌。在超微结构上,中膜蜕膜中的滋养细胞与脱落膜碎片的内皮细胞紧密接触。这些发现表明,α2M以及由此生物利用度受α2M调节的蛋白酶和/或细胞因子对滋养细胞的侵袭具有重要的决定性调节作用。

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