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Single-cell reconstruction of the early maternal-fetal interface in humans

机译:人类早期母胎界面的单细胞重建

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During early human pregnancy the uterine mucosa transforms into the decidua, into which the fetal placenta implants and where placental trophoblast cells intermingle and communicate with maternal cells. Trophoblast-decidual interactions underlie common diseases of pregnancy, including pre-eclampsia and stillbirth. Here we profile the transcriptomes of about 70,000 single cells from first-trimester placentas with matched maternal blood and decidual cells. The cellular composition of human decidua reveals subsets of perivascolar and stromal cells that are located in distinct decidual layers. There are three major subsets of decidual natural killer cells that have distinctive immunomodulatory and chemokine profiles. We develop a repository of ligand-receptor complexes and a statistical tool to predict the cell-type specificity of cell-cell communication via these molecular interactions. Our data identify many regulatory interactions that prevent harmful innate or adaptive immune responses in this environment. Our single-cell atlas of the maternal-fetal interface reveals the cellular organization of the decidua and placenta, and the interactions that are critical for placentation and reproductive success.
机译:在人类早期怀孕期间,子宫粘膜转变为蜕膜,胎儿胎盘植入其中,胎盘滋养层细胞与母体细胞混合并连通。滋养层与蜕膜的相互作用是妊娠常见疾病的基础,包括先兆子痫和死胎。在这里,我们剖析了妊娠早期胎盘中约70,000个单细胞的转录组,以及匹配的母血和蜕膜细胞。人蜕膜的细胞组成揭示了位于不同蜕膜层的周细胞和基质细胞的子集。蜕膜自然杀伤细胞主要分为三个亚组,它们具有独特的免疫调节和趋化因子特征。我们开发了一个配体-受体复合物和统计工具来预测通过这些分子相互作用的细胞间通信的细胞类型特异性的资料库。我们的数据确定了许多调节相互作用,可以阻止这种环境下有害的先天或适应性免疫反应。我们的母胎界面单细胞图谱揭示了蜕膜和胎盘的细胞结构,以及对胎盘和生殖成功至关重要的相互作用。

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