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早孕期绒毛和蜕膜组织人类滋养细胞的全基因组表达谱。

Genome-wide expression profile of first trimester villous and extravillous human trophoblast cells.

机构信息

Department of Pathology and Centre for Trophoblast Research, University of Cambridge, Tennis Court Road, Cambridge CB2 1QP, UK.

出版信息

Placenta. 2011 Jan;32(1):33-43. doi: 10.1016/j.placenta.2010.10.010. Epub 2010 Nov 13.

Abstract

We have examined the transcriptional changes associated with differentiation from villous to extravillous trophoblast using a whole genome microarray. Villous trophoblast (VT) is in contact with maternal blood and mediates nutrient exchange whereas extravillous trophoblast (EVT) invades the decidua and remodels uterine arteries. Using highly purified first trimester trophoblast we identified over 3000 transcripts that are differentially expressed. Many of these transcripts represent novel functions and pathways that show co-ordinated up-regulation in VT or EVT. In addition we identify new players in established functions such as migration, immune modulation and cytokine or angiogenic factor secretion by EVT. The transition from VT to EVT is also characterised by alterations in transcription factors such as STAT4 and IRF9, which may co-ordinate these changes. Transcripts encoding several members of the immunoglobulin-superfamily, which are normally expressed on leukocytes, were highly transcribed in EVT but not expressed as protein, indicating specific control of translation in EVT. Interactions of trophoblast with decidual leukocytes are involved in regulating EVT invasion. We show that decidual T-cells, macrophages and NK cells express the inhibitory collagen receptor LAIR-1 and that EVT secrete LAIR-2, which can block this interaction. This represents a new mechanism by which EVT can modulate leukocyte function in the decidua. Since LAIR-2 is detectable in the urine of pregnant, but not non-pregnant women, trophoblast-derived LAIR-2 may also have systemic effects during pregnancy.

摘要

我们使用全基因组微阵列检查了绒毛向绒毛外滋养层分化相关的转录变化。绒毛滋养层(VT)与母体血液接触并介导营养交换,而绒毛外滋养层(EVT)则侵入蜕膜并重塑子宫动脉。使用高度纯化的早孕滋养层,我们鉴定出 3000 多个差异表达的转录本。其中许多转录本代表新的功能和途径,在 VT 或 EVT 中表现出协调上调。此外,我们还确定了在迁移、免疫调节和 EVT 分泌细胞因子或血管生成因子等既定功能中的新参与者。从 VT 到 EVT 的转变还表现为转录因子如 STAT4 和 IRF9 的改变,它们可能协调这些变化。编码免疫球蛋白超家族几个成员的转录本在 EVT 中高度转录,但不表达为蛋白质,这表明 EVT 中翻译的特异性控制。滋养层与蜕膜白细胞的相互作用参与调节 EVT 的浸润。我们表明,蜕膜 T 细胞、巨噬细胞和 NK 细胞表达抑制性胶原受体 LAIR-1,而 EVT 分泌 LAIR-2,可阻断这种相互作用。这代表了 EVT 可以调节蜕膜中白细胞功能的新机制。由于 LAIR-2 在孕妇尿液中可检测到,但在非孕妇尿液中不可检测到,因此滋养层衍生的 LAIR-2 也可能在怀孕期间具有全身作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f196/3065343/c03c2723e4a2/gr1.jpg

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