首页> 外文期刊>AJRI: American Journal of Reproductive Immunology >A unique preliminary study on placental apoptosis in mice with passive immunization of anti-phosphatidylethanolamine antibodies and anti-factor XII antibodies.
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A unique preliminary study on placental apoptosis in mice with passive immunization of anti-phosphatidylethanolamine antibodies and anti-factor XII antibodies.

机译:用抗磷脂酰乙醇胺抗体和抗XII抗体被动免疫对小鼠胎盘凋亡进行的独特的初步研究。

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PROBLEM: Antiphospholipid antibodies have been investigated both in humans and in animal models. In contrast, there are fewer reports describing anti-phosphatidylethanolamine (aPE) antibodies in humans, and there are no reports of animal studies with aPE till date. Clinically, FXII deficiency or anti-FXII antibodies are sometimes associated with aPE in patients with recurrent pregnancy loss. Therefore, we asked whether aPE and/or anti-FXII in mice could cause fetal resorption, placental thrombosis and apoptosis. Moreover, antibodies to respective target antigens (LDC27 or IPP30) could cause pregnancy failure as well. METHODS OF STUDY: Animal models were used to carry out these objectives. All the animals were immunized with different antibodies by passive immunization. Placental samples were used for various observations. RESULTS AND CONCLUSIONS: Mice with passive immunization of aPE (or anti-LDC27) and aFXII (or anti-IPP30) produced a slight increase in fetal resorption, but markedly induced thrombosis and hemorrhage in the placenta associated with lower platelet counts and increased placental apoptosis. In addition, fewer mitotic cells, less trophoblast giant cell invasion, and more shrunken cells in the deciduas were seen. Our study supports the pathogenic role of aPE and aFXII in pregnancy complications and also suggests a beneficial role of LDC27 and IPP30 antigens on pregnancy failures.
机译:问题:抗磷脂抗体已在人类和动物模型中进行了研究。相比之下,关于抗磷脂酰乙醇胺(aPE)抗体在人体中的报道较少,迄今为止,还没有关于使用aPE进行动物研究的报道。在临床上,FXII缺乏症或抗FXII抗体有时与复发性流产患者中的aPE相关。因此,我们询问小鼠中的aPE和/或抗FXII是否会引起胎儿吸收,胎盘血栓形成和细胞凋亡。此外,针对各个靶抗原(LDC27或IPP30)的抗体也可能导致妊娠失败。研究方法:动物模型被用来实现这些目标。通过被动免疫用不同的抗体免疫所有动物。胎盘样本用于各种观察。结果与结论:被动免疫aPE(或抗LDC27)和aFXII(或抗IPP30)的小鼠可使胎儿的吸收略有增加,但显着诱导胎盘血栓形成和出血,降低血小板计数并增加胎盘凋亡。另外,在十足动物中观察到更少的有丝分裂细胞,更少的滋养层巨细胞入侵和更多的收缩细胞。我们的研究支持aPE和aFXII在妊娠并发症中的致病作用,并且还提出了LDC27和IPP30抗原对妊娠失败的有益作用。

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