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子痫前期:当婴儿为小于胎龄儿时,与合体细胞凋亡增加有关。

Pre-eclampsia: associated with increased syncytial apoptosis when the infant is small-for-gestational-age.

作者信息

Austgulen Rigmor, Isaksen Christina Vogt, Chedwick Lisa, Romundstad Pål, Vatten Lars, Craven Catherine

机构信息

Faculty of Medicine, Institute of Cancer Research and Molecular Medicine, Norwegian University of Science and Technology, 7489 Trondheim, Norway.

出版信息

J Reprod Immunol. 2004 Feb;61(1):39-50. doi: 10.1016/j.jri.2003.10.001.

Abstract

The present investigation was undertaken to study the association between placental apoptosis and pre-eclampsia, discriminating between pre-eclamptic pregnancies with appropriate-, and small-for-gestational-age (SGA), infants. Twenty pregnancies with pre-eclampsia and SGA (birth weight at or below -2 standard deviations) infants were selected in a retrospective study. Subsequently, corresponding numbers of gestational age-matched pre-eclampsia cases with appropriate-gestational-age (AGA) (birth weight at or above the 50% centile) infants and AGA controls without pre-eclampsia were selected. Formalin-fixed placental tissue was obtained from all groups. Apoptosis was assessed by a monoclonal antibody (M30), detecting a neoepitope of cytokeratin that is generated early in the apoptotic cascade. M30-positive cells were counted in villous and decidual/ basal plate tissue fields, and results were given as numbers of M30-positive cells per field. The study was performed blinded. Increased apoptosis was found in the syncytiotrophoblast layer in pre-eclampsia with SGA infants (0.14 apototic incidents per field of villous tissue, with 0.04-0.23 as the corresponding 25-75% inter quartile range (IQR) (P=0.05)). Syncytial apoptosis in the syncytial layer in the pre-eclampsia group with AGA infants was lower (0.09, IQR 0.03-0.15) and corresponded to the level detected among controls (0.06, IQR 0.03-0.17). Apoptosis in other placental cellular compartments did not differ between groups. The increased syncytial apoptosis found in placentas from pregnancies with SGA infants may either be due to specific mechanisms associated with pre-eclampsia complicated with growth restriction, or may simply reflect the presence of syncytiotrophoblast layer damage, regardless of underlying pathological condition.

摘要

本研究旨在探讨胎盘细胞凋亡与子痫前期之间的关联,并区分胎儿发育正常和小于胎龄(SGA)的子痫前期妊娠。在一项回顾性研究中,选取了20例患有子痫前期且胎儿为SGA(出生体重在或低于-2标准差)的妊娠病例。随后,选取了相应数量的孕周匹配、胎儿发育正常(AGA)(出生体重在第50百分位数及以上)的子痫前期病例以及无子痫前期的AGA对照。所有组均获取了经福尔马林固定的胎盘组织。通过一种单克隆抗体(M30)评估细胞凋亡,该抗体可检测细胞角蛋白的一个新表位,此表位在凋亡级联反应早期产生。对绒毛和蜕膜/基底板组织区域中的M30阳性细胞进行计数,结果以每视野M30阳性细胞数表示。该研究采用盲法进行。在伴有SGA胎儿的子痫前期患者的合体滋养层中发现细胞凋亡增加(每视野绒毛组织的凋亡事件为0.14,相应的四分位间距(IQR)为25%-75%,即0.04-0.23,P=0.05)。伴有AGA胎儿的子痫前期组合体层中的合体细胞凋亡较低(0.09,IQR 0.03-0.15),与对照组检测到的水平相当(0.06,IQR 0.03-0.17)。各胎盘细胞区室的凋亡在组间无差异。在SGA胎儿妊娠的胎盘中发现的合体细胞凋亡增加,可能是由于与子痫前期并发生长受限相关的特定机制,也可能仅仅反映了合体滋养层的损伤,而与潜在的病理状况无关。

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