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首页> 外文期刊>Journal of Leukocyte Biology: An Official Publication of the Reticuloendothelial Society >Frontline Science: Myeloid-derived suppressor cells (MDSCs) facilitate maternal-fetal tolerance in mice
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Frontline Science: Myeloid-derived suppressor cells (MDSCs) facilitate maternal-fetal tolerance in mice

机译:Frontline Science:骨髓衍生的抑制细胞(MDSCs)促进小鼠的母体胎儿耐受性

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摘要

During successful pregnancy, a woman is immunologically tolerant of her genetically and antigenically disparate fetus, a state known as maternal-fetal tolerance. How this state is maintained has puzzled investigators for more than half a century. Diverse, immune and nonimmune mechanisms have been proposed; however, these mechanisms appear to be unrelated and to act independently. A population of immune suppressive cells called myeloid-derived suppressor cells (MDSCs) accumulates in pregnant mice and women. Given the profound immune suppressive function of MDSCs, it has been suggested that this cell population may facilitate successful pregnancy by contributing to maternal-fetal tolerance. We now report that myeloid cells with the characteristics of MDSCs not only accumulate in the circulation and uterus of female mice following mating but also suppress T cell activation and function in pregnant mice. Depletion of cells with the phenotype and function of MDSCs from gestation d 0.5 through d 7.5 resulted in implantation failure, increased T cell activation, and increased T cell infiltration into the uterus, whereas induction of MDSCs restored successful pregnancy and reduced T cell activation. MDSC-mediated suppression during pregnancy was accompanied by the down-regulation of L-selectin on naive T cells and a reduced ability of naive T cells to enter lymph nodes and become activated. Because MDSCs regulate many of the immune and nonimmune mechanisms previously attributed to maternal-fetal tolerance, MDSCs may be a unifying mechanism promoting maternal-fetal tolerance, and their induction may facilitate successful pregnancy in women who spontaneously abort or miscarry because of dysfunctional maternal-fetal tolerance.
机译:在成功怀孕期间,一个女人在遗传和抗原的胎儿的免疫学上耐受,称为母体胎儿的状态。这种国家的维护方式如何令人困惑的调查人员超过半个世纪。提出了不同,免疫和非免疫机制;但是,这些机制似乎不相关并独立行动。一种称为霉菌衍生的抑制细胞(MDSC)的免疫抑制细胞群在怀孕的小鼠和女性中积累。鉴于MDSCS的深刻免疫抑制功能,已经提出这种细胞群可以通过促进母体含耐量来促进成功怀孕。我们现在举报的骨髓细胞不仅在交配后的雌性小鼠的循环和子宫内积聚,而且抑制了在怀孕小鼠中的循环和子宫内积聚。通过从妊娠D.5至D 7.5脱离MDSCs的表型和功能的细胞耗尽导致植入失败,增加T细胞活化,并将T细胞浸润增加进入子宫,而MDSCS诱导成功妊娠和降低的T细胞活化。妊娠期间的MDSC介导的抑制伴随着L-SELETIN对幼稚T细胞的下调和幼稚T细胞进入淋巴结的能力降低并被激活。由于MDSCS调节以前归因于母体胎儿耐受的许多免疫和非免疫机制,因此MDSC可能是促进母胎耐受性的统一机制,并且由于功能障碍的母性胎儿,他们的诱导可能促进成功怀孕。由于功能障碍的母性胎儿宽容。

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