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Differential Triiodothyronine Responsiveness and Transport by Human Cytotrophoblasts from Normal and Growth-Restricted Pregnancies

机译:正常和生长受限妊娠的人滋养细胞对三碘甲状腺氨酸的响应和转运差异。

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摘要

>Context: Abnormal placentation in human pregnancy is associated with intrauterine fetal growth restriction (IUGR). Our group has previously reported the association between severe IUGR, lower fetal circulating concentrations of thyroid hormones (THs), and altered expression of TH receptors and TH transporters within human placental villi. We postulate that altered TH bioavailability to trophoblasts may contribute to the pathogenesis of IUGR.>Design and Objective: Cytotrophoblasts were isolated from normal and IUGR human placentae to compare their responsiveness to T3 and their capability for T3 transport.>Results: Compared with normal cytotrophoblasts, the viability of IUGR cytotrophoblasts (assessed by methyltetrazoleum assay) was significantly reduced (P < 0.001), whereas apoptosis (assessed using caspase 3/7 activity and M30 immunoreactivity) was significantly increased after T3 treatment for 48 h (P < 0.001 and P < 0.01, respectively). The secretion of human chorionic gonadotropin was significantly increased by IUGR cytotrophoblasts compared with normal cytotrophoblasts (P < 0.001), independently of T3 treatment. Net transport of [125I]T3 was 20% higher by IUGR cytotrophoblasts compared with normal cytotrophoblasts (P < 0.001), and this was accompanied by a 2-fold increase in the protein expression of the TH transporter, monocarboxylate transporter 8, as assessed by Western immunoblotting (P < 0.01).>Conclusions: IUGR cytotrophoblasts demonstrate altered responsiveness to T3 with significant effects on cell survival and apoptosis compared with normal cytotrophoblasts. Increased monocarboxylate transporter 8 expression and intracellular T3 accumulation may contribute to the altered T3 responsiveness of IUGR cytotrophoblasts.
机译:>背景:人类妊娠中的胎盘异常与宫内胎儿生长受限(IUGR)有关。我们的研究小组以前曾报道过严重的IUGR,胎儿的甲状腺激素循环浓度降低以及人胎盘绒毛中TH受体和TH转运蛋白表达的改变之间的相关性。我们推测,滋养层细胞TH的生物利用度变化可能与IUGR的发病有关。>设计与目的:从正常胎盘和IUGR人胎盘中分离出滋养细胞,以比较它们对T3的反应性及其对T3转运的能力。 strong>结果:与正常的细胞滋养细胞相比,IUGR的细胞滋养细胞(通过甲基四氮唑测定评估)的活力显着降低(P <0.001),而凋亡(使用caspase 3/7活性和M30免疫反应性评估)则明显增加T3处理48小时后(分别为P <0.001和P <0.01)。与正常的细胞滋养细胞相比,IUGR细胞滋养细胞显着增加了人绒毛膜促性腺激素的分泌(P <0.001),与T3处理无关。与正常的细胞滋养细胞相比,IUGR的细胞滋养细胞对[ 125 I] T3的净转运增加了20%(P <0.001),并且TH转运蛋白的蛋白质表达增加了2倍Western blotting评估单羧酸盐转运蛋白8(P <0.01)。>结论:与正常的细胞滋养细胞相比,IUGR细胞滋养细胞对T3的反应性发生了改变,对细胞存活和细胞凋亡具有显着影响。单羧酸转运蛋白8表达的增加和细胞内T3积累可能有助于改变IUGR滋养细胞的T3反应性。

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