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Lower FOXP3 mRNA Expression in First-Trimester Decidual Tissue from Uncomplicated Term Pregnancies with a Male Fetus

机译:单纯性足月妊娠男性胎儿早孕蜕膜组织中较低的FOXP3 mRNA表达

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摘要

Pregnancies with a male fetus are associated with higher risks of pregnancy complications through maladaptation of the maternal immune system. The pathophysiology of this phenomenon is unknown. A possible pathway could be a fetal sex-dependent maternal immune response, since males have a Y chromosome encoding specific allogenic proteins, possibly contributing to a different response and higher complication risks. To analyze whether fetal sex affects mRNA expression of maternal immune genes in early pregnancy, real-time PCR quantification was performed in the decidual tissue from primigravid pregnancies (n = 20) between 10 and 12 weeks with uncomplicated term outcomes. Early-pregnancy decidual mRNA expression of the regulatory T-cell marker, FOXP3, was sixfold lower (p < 0.01) in pregnancies with a male fetus compared to pregnancies with a female fetus. Additionally, mRNA expression of IFNγ was sixfold (p < 0.05) lower in pregnancies with a male fetus. The present data imply maternal immunologic differences between pregnancies with male and female fetuses which could be involved in different pregnancy pathophysiologic outcomes. Moreover, this study indicates that researchers in reproductive immunology should always consider fetal sex bias.
机译:通过母体免疫系统的适应不良,男性胎儿怀孕与妊娠并发症的高风险相关。这种现象的病理生理学是未知的。一种可能的途径可能是胎儿性别依赖性的母体免疫反应,因为男性具有编码特定同种异体蛋白的Y染色体,可能导致不同的反应和更高的并发症风险。为了分析胎儿性别是否在怀孕初期影响母体免疫基因的mRNA表达,在初次妊娠(n = 20)的蜕膜组织中进行了10到12周的实时PCR定量分析,并得出简单的足月结局。男性胎儿的妊娠早期调节性T细胞标志物FOXP3的蜕膜mRNA表达比女性胎儿低六倍(p <0.01)。此外,在男性胎儿中,IFNγ的mRNA表达降低了六倍(p <0.05)。目前的数据表明,男女胎儿妊娠的母体免疫学差异可能与不同的妊娠病理生理结果有关。此外,这项研究表明生殖免疫学研究人员应始终考虑胎儿性别偏见。

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