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因 137Cs 摄入导致的胎盘损伤的形态学和免疫组织化学特征

MORPHOLOGICAL AND IMMUNOHISTOCHEMICAL FEATURES OF PLACENTAL DAMAGE DUE TO THE INCORPORATION OF 137Cs.

机构信息

State Institution Institute of Pediatrics, Obstetrics, and Gynecology named after Academician О. M. Lukyanova of the National Аcademy of Мedical Sciences of Ukraine, 8 Platona Mayborody St., Kyiv, 04050, Ukraine.

出版信息

Probl Radiac Med Radiobiol. 2022 Dec;27:474-494. doi: 10.33145/2304-8336-2022-27-474-494.

Abstract

OBJECTIVE

to investigate the morphological and immunohistochemical features of placental damage due to theincorporation of 137Cs depending on the scenario of pregnancy completion.

MATERIALS AND METHODS

The study material consisted of placentas from 60 women with reproductive losses inanamnesis and signs of termination of the current pregnancy (first group) and placental samples from 30 women with an uncomplicated gestation and an unencumbered anamnesis (control group). The detailed study required the distribution of placental samples from the first group into subgroups. Subgroup 1a included 38 placentas from women who gave birth at 37-40 weeks, despite signs of termination of the current pregnancy. Subgroup 1b - placentas of 13 women who gave birth at a gestation period of 28-36 weeks + 6 days. Subgroup 1c - 9 placental samples from women who gave birth at a gestation period of 22-27 weeks + 6 days. The volumetric activity of the 137Cs in the placentas was measured using β-spectrometer. The histology of the placenta was studied using a standard technique. The following expressions were studied in placenta: CD31 / PECAM-1, CD45 / T200 / LCA, CD56 / NCAM-1, CEA / CD66e Ab-2, Vimentin, using indirect streptavidin peroxidase detection method.

RESULTS

Placentas accumulate 137Cs. The different volumetric activity of the isotope correlates with scenarios of pregnancy. Due to the action of incorporated 137Cs with a specific mass of more than 1.1 Bq/kg, placental dysfunction develops. The consequences of placental dysfunction depend on the volumetric activity of the 137Cs and the preservation of adaptive and compensatory reactions in the placenta. Morphological and immunohistochemical features of placental damage to incorporated 137Cs were established, depending on the scenario of completion of pregnancy. A marker of unfavorable completion of pregnancy is the expression of a carcinoembryonic antigen (CEA) in the placenta.

CONCLUSIONS

Premature termination of pregnancy (PTP) is a multifactorial pathology associated with pathological changes in immune and neuroendocrine regulation and hereditary, infectious, and environmental factors that disrupt the adaptation mechanisms in the mother-placenta-fetus system. Intraplacental irradiation of 137Cs is one of the factors in the multifactorial nature of reproductive losses. As a result of intraplacental irradiation of 137Cs, the architecture of the placenta is disturbed, the activity of pro-inflammatory cytokines CD45 and CD56 increases, and the coagulation cascade is activated. Extreme effects depend on the volumetric activity of the isotope incorporated in the placenta and the organ's compensatory capacity. Accumulation of up to 1.0 Bq/kg 137Cs does not affect the course of gestation. Internal irradiation with an activity of 4.5-10.4 Bq/kg 137Cs triggers late preterm labor. The nature of the damages corresponds to the category of «lesion of the maternal stroma» of the placenta. The volumetric activity of 137Cs over 10.4 Bq/kg is a probable cause of early preterm labor and antenatal fetal death. At the same time, the maternal and fetal structures of the placenta suffer damage. Expression of vimentin is a marker of placental destruction due to internal irradiation of 137Cs with a specific gravity of more than 4.5 Bq/kg. Expression of CEA in the structures of the placenta of women with PTP is a unique find and marker of premature birth and antenatal fetal death with intraplacental irradiation of 137Cs with an activity of more than 4.5 Bq/kg.

摘要

目的

研究 137Cs 摄入导致胎盘损伤的形态学和免疫组织化学特征,具体取决于妊娠完成的情况。

材料与方法

本研究材料由 60 名有生殖损失病史且当前妊娠终止迹象的女性的胎盘(第一组)和 30 名妊娠正常且无病史的女性的胎盘样本(对照组)组成。详细的研究需要将第一组的胎盘样本分成亚组。亚组 1a 包括 38 名在 37-40 周分娩的女性的胎盘,尽管有当前妊娠终止的迹象。亚组 1b 包括 13 名在 28-36 周+6 天分娩的女性的胎盘。亚组 1c 包括 9 名在 22-27 周+6 天分娩的女性的胎盘样本。使用β谱仪测量胎盘内 137Cs 的体积活性。使用标准技术研究胎盘的组织学。在胎盘内研究了以下表达:CD31/PECAM-1、CD45/T200/LCA、CD56/NCAM-1、CEA/CD66e Ab-2、波形蛋白,使用间接链霉亲和素过氧化物酶检测方法。

结果

胎盘会积累 137Cs。同位素的不同体积活性与妊娠完成情况相关。由于特定质量超过 1.1 Bq/kg 的 137Cs 的作用,胎盘功能障碍会发展。胎盘功能障碍的后果取决于 137Cs 的体积活性以及胎盘内适应性和代偿性反应的保留情况。根据妊娠完成情况,建立了胎盘对摄入 137Cs 的形态学和免疫组织化学损伤特征。不利妊娠完成的标志物是胎盘中癌胚抗原(CEA)的表达。

结论

早产(PTP)是一种多因素疾病,与免疫和神经内分泌调节的病理变化以及遗传、感染和环境因素有关,这些因素破坏了母婴胎盘胎儿系统的适应机制。137Cs 胎盘内照射是生殖损失多因素性质的因素之一。由于 137Cs 胎盘内照射,胎盘结构受到干扰,促炎细胞因子 CD45 和 CD56 的活性增加,凝血级联被激活。极端影响取决于胎盘内掺入的同位素的体积活性和器官的代偿能力。积累量达到 1.0 Bq/kg 以下的 137Cs 不会影响妊娠过程。活性为 4.5-10.4 Bq/kg 的内照射会引发晚期早产。损伤的性质与胎盘“母体基质损伤”的类别相对应。体积活性超过 10.4 Bq/kg 的 137Cs 可能是早期早产和产前胎儿死亡的原因。同时,胎盘的母体和胎儿结构都会受到损伤。波形蛋白的表达是胎盘因内照射 137Cs 而破坏的标志物,比重大于 4.5 Bq/kg。在胎盘内照射 137Cs 活性超过 4.5 Bq/kg 的情况下,胎盘结构中 CEA 的表达是早产和产前胎儿死亡的独特发现和标志物。

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