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MEHP 对人胎儿睾丸和卵巢中 LXRα 的细胞和分子作用。

Cellular and molecular effect of MEHP Involving LXRα in human fetal testis and ovary.

机构信息

University Paris Diderot, Sorbonne Paris Cité, Laboratory of Development of the Gonads, Unit of Stem Cells and Radiation, Fontenay-aux-Roses, France.

出版信息

PLoS One. 2012;7(10):e48266. doi: 10.1371/journal.pone.0048266. Epub 2012 Oct 30.

Abstract

BACKGROUND

Phthalates have been shown to have reprotoxic effects in rodents and human during fetal life. Previous studies indicate that some members of the nuclear receptor (NR) superfamilly potentially mediate phthalate effects. This study aimed to assess if expression of these nuclear receptors are modulated in the response to MEHP exposure on the human fetal gonads in vitro.

METHODOLOGY/PRINCIPAL FINDINGS: Testes and ovaries from 7 to 12 gestational weeks human fetuses were exposed to 10(-4)M MEHP for 72 h in vitro. Transcriptional level of NRs and of downstream genes was then investigated using TLDA (TaqMan Low Density Array) and qPCR approaches. To determine whether somatic or germ cells of the testis are involved in the response to MEHP exposure, we developed a highly efficient cytometric germ cell sorting approach. In vitro exposure of fetal testes and ovaries to MEHP up-regulated the expression of LXRα, SREBP members and of downstream genes involved in the lipid and cholesterol synthesis in the whole gonad. In sorted testicular cells, this effect is only observable in somatic cells but not in the gonocytes. Moreover, the germ cell loss induced by MEHP exposure, that we previously described, is restricted to the male gonad as oogonia density is not affected in vitro.

CONCLUSIONS/SIGNIFICANCE: We evidenced for the first time that phthalate increases the levels of mRNA for LXRα, and SREBP members potentially deregulating lipids/cholesterol synthesis in human fetal gonads. Interestingly, this novel effect is observable in both male and female whereas the germ cell apoptosis is restricted to the male gonad. Furthermore, we presented here a novel and potentially very useful flow cytometric cell sorting method to analyse molecular changes in germ cells versus somatic cells.

摘要

背景

已有研究表明邻苯二甲酸酯在胎儿期对啮齿动物和人类具有生殖毒性作用。先前的研究表明,核受体(NR)超家族的某些成员可能介导邻苯二甲酸酯的作用。本研究旨在评估 MEHP 暴露是否会调节体外人胎儿性腺中这些核受体的表达。

方法/主要发现:将 7 至 12 孕周人胎儿的睾丸和卵巢在体外暴露于 10(-4)M MEHP 中 72 小时。然后使用 TLDA(TaqMan 低密度阵列)和 qPCR 方法研究 NR 和下游基因的转录水平。为了确定睾丸的体细胞或生殖细胞是否参与 MEHP 暴露的反应,我们开发了一种高效的细胞分选方法。MEHP 体外暴露于胎儿睾丸和卵巢中,上调了整个性腺中 LXRα、SREBP 成员以及参与脂质和胆固醇合成的下游基因的表达。在分选的睾丸细胞中,这种效应仅在体细胞中可见,而在精原细胞中不可见。此外,我们之前描述的 MEHP 暴露诱导的生殖细胞丢失仅发生在雄性性腺中,因为体外卵母细胞密度不受影响。

结论/意义:我们首次证明邻苯二甲酸酯增加了 LXRα 和 SREBP 成员的 mRNA 水平,可能会使人类胎儿性腺中的脂质/胆固醇合成失调。有趣的是,这种新的作用在雄性和雌性中都可见,而生殖细胞凋亡仅限于雄性性腺。此外,我们在此介绍了一种新的、可能非常有用的流式细胞术细胞分选方法,用于分析生殖细胞与体细胞之间的分子变化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d813/3484128/e23f9bc6a7a6/pone.0048266.g001.jpg

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