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人类胚胎干细胞及其体外分化为胎盘祖细胞过程中存在性别特异性基因表达差异。

Sex-Specific Gene Expression Differences Are Evident in Human Embryonic Stem Cells and During In Vitro Differentiation of Human Placental Progenitor Cells.

机构信息

1 Department of Biomedical Sciences, School of Veterinary Medicine, University of Pennsylvania , Philadelphia, Pennsylvania.

2 Department of Pathobiology, School of Veterinary Medicine, University of Pennsylvania , Philadelphia, Pennsylvania.

出版信息

Stem Cells Dev. 2018 Oct 1;27(19):1360-1375. doi: 10.1089/scd.2018.0081. Epub 2018 Aug 21.

Abstract

The placenta is a short-lived tissue required for embryonic growth and survival, and it is fetal derived. Fetal sex influences gestation, and many sexual dimorphic diseases have origins in utero. There is sex-biased gene expression in third-trimester human placentas, yet the origin of sex-specific expression is unknown. Here, we used an in vitro differentiation model to convert human embryonic stem cells (hESCs) into trophoblastic progenitor cells of the first-trimester placenta, which will eventually become mature extravillous trophoblasts and syncytiotrophoblasts. We observed significant sex differences in transcriptomic profiles of hESCs and trophoblastic progenitors, and also with the differentiation process itself. Male cells had higher dosage of X/Y gene pairs relative to female samples, supporting functions for Y-linked genes beyond spermatogenesis in the hESCs and in the early placenta. Female-specific differentiation altered the expression of several thousand genes compared with male cells, and female cells specifically upregulated numerous autosomal genes with known roles in trophoblast function. Sex-biased upregulation of cellular pathways during trophoblast differentiation was also evident. This study is the first to identify sex differences in trophoblastic progenitor cells of the first-trimester human placenta, and reveal early origins for sexual dimorphism.

摘要

胎盘是一种短暂存在的组织,对于胚胎的生长和存活至关重要,且来源于胎儿。胎儿性别会影响妊娠过程,许多性二态性疾病都起源于子宫内。在人类胎盘的第三个 trimester 中存在着性别偏向的基因表达,但性别特异性表达的起源尚不清楚。在这里,我们使用体外分化模型将人类胚胎干细胞(hESC)转化为第一个 trimester 胎盘的滋养层祖细胞,这些细胞最终将成为成熟的绒毛外滋养层和合体滋养层。我们观察到 hESC 和滋养层祖细胞的转录组谱以及分化过程本身存在显著的性别差异。与女性样本相比,男性细胞中 X/Y 基因对的剂量更高,这支持了 Y 连锁基因在 hESC 中和早期胎盘中的作用超出了精子发生。与男性细胞相比,女性细胞的分化特异性改变了数千个基因的表达,并且女性细胞特异性地上调了许多具有已知在滋养层功能中作用的常染色体基因。在滋养层分化过程中细胞途径的性别偏向性上调也很明显。这项研究首次鉴定了第一个 trimester 人类胎盘滋养层祖细胞中的性别差异,并揭示了性二态性的早期起源。

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