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Bisphenol A Exposure Alters Developmental Gene Expression in the Fetal Rhesus Macaque Uterus

机译:双酚A暴露改变胎儿恒河猴猕猴的发育基因表达。

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摘要

Bisphenol A (BPA) exposure results in numerous developmental and functional abnormalities in reproductive organs in rodent models, but limited data are available regarding BPA effects in the primate uterus. To determine if maternal oral BPA exposure affects fetal uterine development in a non-human primate model, pregnant rhesus macaques carrying female fetuses were exposed orally to 400 µg/kg BPA or vehicle control daily from gestation day (GD) 50–100 or GD100–165. Fetal uteri were collected at the completion of treatment (GD100 or GD165); tissue histology, cell proliferation, and expression of estrogen receptor alpha (ERα) and progesterone receptor (PR) were compared to that of controls. Gene expression analysis was conducted using rhesus macaque microarrays. There were no significant differences in histology or in the percentage of cells expressing the proliferation marker Ki-67, ERα, or PR in BPA-exposed uteri compared to controls at GD100 or GD165. Minimal differences in gene expression were observed between BPA-exposed and control GD100 uteri. However, at GD165, BPA-exposed uteri had significant differences in gene expression compared to controls. Several of the altered genes, including HOXA13, WNT4, and WNT5A, are critical for reproductive organ development and/or adult function. We conclude that second or third trimester BPA exposure does not significantly affect fetal uterus development based on morphological, proliferation, and steroid hormone receptor assessments. However, differences in expression of key developmental genes after third trimester exposure suggest that BPA could alter transcriptional signals influencing uterine function later in life.
机译:在啮齿动物模型中,双酚A(BPA)暴露会导致生殖器官出现许多发育和功能异常,但关于BPA在灵长类动物子宫中的作用的可用数据有限。为了确定在非人类灵长类动物模型中母亲口服BPA暴露是否会影响胎儿子宫发育,从妊娠日(GD)50–100或GD100– 165。治疗结束时收集胎儿子宫(GD100或GD165)。将组织组织学,细胞增殖以及雌激素受体α(ERα)和孕激素受体(PR)的表达与对照组进行比较。使用恒河猴猕猴微阵列进行基因表达分析。与在GD100或GD165的对照组相比,在暴露于BPA的子宫中,组织学或表达增殖标记Ki-67,ERα或PR的细胞百分比无显着差异。暴露于双酚A和对照GD100子宫之间的基因表达差异最小。然而,与对照相比,GD165暴露于BPA的子宫在基因表达上有显着差异。几个改变的基因,包括HOXA13,WNT4和WNT5A,对生殖器官发育和/或成年功能至关重要。我们得出的结论是,根据形态,增殖和类固醇激素受体评估,妊娠中期或中期BPA暴露不会显着影响胎儿子宫的发育。然而,孕晚期暴露后关键发育基因的表达差异表明,BPA可能会改变影响生命后期子宫功能的转录信号。

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