首页> 美国卫生研究院文献>International Journal of Molecular Sciences >MiR-519d-3p in Trophoblastic Cells: Effects Targets and Transfer to Allogeneic Immune Cells via Extracellular Vesicles
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MiR-519d-3p in Trophoblastic Cells: Effects Targets and Transfer to Allogeneic Immune Cells via Extracellular Vesicles

机译:滋养细胞中的MiR-519d-3p:作用靶点和通过细胞外囊泡转移至同种异体免疫细胞

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摘要

Members of the placenta-specific miRNA cluster C19MC, including miR-519d, are secreted by fetal trophoblast cells within extracellular vesicles (EVs). Trophoblast-derived EVs can be internalized by the autologous trophoblast and surrounding maternal immune cells, resulting in coordination of cellular responses. The study of functions and targets of placental miRNAs in the donor and recipient cells may contribute to the understanding of the immune tolerance essential in pregnancy. Here, we report that miR-519d-3p levels correlate positively with cell proliferation and negatively with migration in trophoblastic cell lines. Inhibition of miR-519d-3p in JEG-3 cells increases caspase-3 activation and apoptosis. PDCD4 and PTEN are targeted by miR-519d-3p in a cell type-specific manner. Transfection of trophoblastic cell lines with miR-519d mimic results in secretion of EVs containing elevated levels of this miRNA (EV ). Autologous cells enhance their proliferation and decrease their migration ability when treated with EV . NK92 cells incorporate EV-delivered miR-519d-3p at higher levels than Jurkat T cells. EV increases the proliferation of Jurkat T cells but decreases that of NK92 cells. Altogether, miR-519d-3p regulates pivotal trophoblast cell functions, can be transferred horizontally via EVs to maternal immune cells and exerts functions therein. Vesicular miRNA transfer from fetal trophoblasts to maternal immune cells may contribute to the immune tolerance in pregnancy.
机译:胎盘特异性miRNA簇C19MC的成员,包括miR-519d,是由细胞外囊泡(EVs)中的胎儿滋养细胞分泌的。滋养细胞来源的电动汽车可被自体滋养细胞和周围的母体免疫细胞内化,从而导致细胞反应的协调。对供体和受体细胞中胎盘miRNA的功能和靶标的研究可能有助于理解妊娠中必不可少的免疫耐受性。在这里,我们报告miR-519d-3p水平与滋养细胞系中的细胞增殖呈正相关,而与滋养细胞系中的迁移呈负相关。在JEG-3细胞中抑制miR-519d-3p会增加caspase-3的激活和凋亡。 miR-519d-3p以细胞类型特异性方式靶向PDCD4和PTEN。用miR-519d模拟物转染滋养细胞细胞系可导致分泌含有高水平这种miRNA(EV)的EV。用EV处理后,自体细胞增强增殖,降低迁移能力。 NK92细胞以比Jurkat T细胞更高的水平掺入EV递送的miR-519d-3p。 EV增加Jurkat T细胞的增殖,但降低NK92细胞的增殖。总而言之,miR-519d-3p调节关键的滋养层细胞功能,可通过电动车水平转移至母体免疫细胞并在其中发挥功能。从胎儿滋养细胞到母体免疫细胞的水泡性miRNA转移可能有助于妊娠期的免疫耐受。

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