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Effects of Bisphenol A and 4-tert-Octylphenol on Embryo Implantation Failure in Mouse

机译:双酚A和4-叔辛基酚对小鼠胚胎植入失败的影响

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摘要

Miscarriage due to blastocyst implantation failure occurs in up to two-thirds of all human miscarriage cases. Calcium ion has been shown to be involved in many cellular signal transduction pathways as well as in the regulation of cell adhesion, which is necessary for the embryo implantation process. Exposure to endocrine-disrupting chemicals (EDs) during early gestation results in disruption of intrauterine implantation and uterine reception, leading to implantation failure. In this study, ovarian estrogen (E2), bisphenol A (BPA), or 4-tert-octylphenol (OP), with or without ICI 182,780 (ICI) were injected subcutaneously from gestation day 1 to gestation day 3 post-coitus. The expression levels of the calcium transport genes were assessed in maternal uteri and implantation sites. The number of implantation sites was significantly low in the OP group, and implantation sites were absent in the E2, ICI and EDs + ICI groups. There were different calcium transient transport channel expression levels in uterus and implantation site samples. The levels of TRPV5 and TRPV6 gene expression were significantly increased by EDs with/without ICI treatment in utero. Meanwhile, TRPV5 and TRPV6 gene expression were significantly lower in implantation sites samples. NCX1 and PMCA1 mRNA levels were significantly decreased by OP and BPA in the implantation site samples. Compared to vehicle treatment in the uterus, both the MUC1 mRNA and protein levels were markedly high in all but the BPA group. Taken together, these results suggest that both BPA and OP can impair embryo implantation through alteration of calcium transport gene expressions and by affecting uterine receptivity.
机译:在所有人类流产病例中,多达三分之二的人因囊胚植入失败而流产。钙离子已经显示出参与许多细胞信号转导途径以及调节细胞粘附,这对于胚胎植入过程是必需的。妊娠早期接触破坏内分泌的化学物质(EDs)会导致子宫内植入和子宫接收中断,从而导致植入失败。在这项研究中,从妊娠第1天到妊娠第3天,皮下注射有或没有ICI 182,780(ICI)的卵巢雌激素(E2),双酚A(BPA)或4-叔辛基苯酚(OP)。在母体子宫和着床部位评估了钙转运基因的表达水平。 OP组的植入位点数量极低,E2,ICI和EDs + ICI组中没有植入位点。子宫和着床部位样本中钙的瞬时转运通道表达水平不同。 EDs宫内/不宫内ICI治疗可显着提高TRPV5和TRPV6基因表达水平。同时,在植入部位样品中TRPV5和TRPV6基因表达显着降低。植入部位样品中的OP和BPA可显着降低NCX1和PMCA1的mRNA水平。与子宫内的媒介物治疗相比,除BPA组外,MUC1 mRNA和蛋白质水平均显着较高。综上所述,这些结果表明,BPA和OP均可通过改变钙转运基因的表达并影响子宫的接受性而损害胚胎着床。

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