首页> 美国卫生研究院文献>PLoS Neglected Tropical Diseases >Alternatively Activated Mononuclear Phagocytes from the Skin Site of Infection and the Impact of IL-4Rα Signalling on CD4+T Cell Survival in Draining Lymph Nodes after Repeated Exposure to Schistosoma mansoni Cercariae
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Alternatively Activated Mononuclear Phagocytes from the Skin Site of Infection and the Impact of IL-4Rα Signalling on CD4+T Cell Survival in Draining Lymph Nodes after Repeated Exposure to Schistosoma mansoni Cercariae

机译:反复感染曼氏血吸虫尾rc后皮肤感染部位的活化的单核吞噬细胞以及IL-4Rα信号对引流淋巴结中CD4 + T细胞存活的影响

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摘要

In a murine model of repeated exposure of the skin to infective Schistosoma mansoni cercariae, events leading to the priming of CD4 cells in the skin draining lymph nodes were examined. The dermal exudate cell (DEC) population recovered from repeatedly (4x) exposed skin contained an influx of mononuclear phagocytes comprising three distinct populations according to their differential expression of F4/80 and MHC-II. As determined by gene expression analysis, all three DEC populations (F4/80-MHC-IIhigh, F4/80+MHC-IIhigh, F4/80+MHC-IIint) exhibited major up-regulation of genes associated with alternative activation. The gene encoding RELMα (hallmark of alternatively activated cells) was highly up-regulated in all three DEC populations. However, in 4x infected mice deficient in RELMα, there was no change in the extent of inflammation at the skin infection site compared to 4x infected wild-type cohorts, nor was there a difference in the abundance of different mononuclear phagocyte DEC populations. The absence of RELMα resulted in greater numbers of CD4+ cells in the skin draining lymph nodes (sdLN) of 4x infected mice, although they remained hypo-responsive. Using mice deficient for IL-4Rα, in which alternative activation is compromised, we show that after repeated schistosome infection, levels of regulatory IL-10 in the skin were reduced, accompanied by increased numbers of MHC-IIhigh cells and CD4+ T cells in the skin. There were also increased numbers of CD4+ T cells in the sdLN in the absence of IL-4Rα compared to cells from singly infected mice. Although their ability to proliferate was still compromised, increased cellularity of sdLN from 4x IL-4RαKO mice correlated with reduced expression of Fas/FasL, resulting in decreased apoptosis and cell death but increased numbers of viable CD4+ T cells. This study highlights a mechanism through which IL-4Rα may regulate the immune system through the induction of IL-10 and regulation of Fas/FasL mediated cell death.
机译:在将皮肤反复暴露于曼氏血吸虫尾c的皮肤中的鼠模型中,检查了导致皮肤引流淋巴结中的CD4细胞启动的事件。从F4 / 80和MHC-II的差异表达中,从反复(4x)暴露的皮肤中回收的真皮渗出液(DEC)群体包含大量包含三个不同群体的单核吞噬细胞。通过基因表达分析确定,所有三个DEC群体(F4 / 80 - MHC-II high ,F4 / 80 + MHC-II < sup> high ,F4 / 80 + MHC-II int )显示出与替代激活相关的基因的主要上调。在所有三个DEC群体中,编码RELMα(交替激活细胞的标志)的基因高度上调。但是,在4x感染的RELMα缺陷小鼠中,与4x感染的野生型队列相比,皮肤感染部位的炎症程度没有变化,不同单核吞噬细胞DEC种群的丰度也没有差异。 RELMα的缺失导致4x感染小鼠皮肤引流淋巴结(sdLN)中的CD4 + 细胞数量增加,尽管它们仍然反应低下。使用缺乏IL-4Rα的小鼠(其中交替激活受到损害),我们发现在反复血吸虫感染后,皮肤中调节性IL-10的水平降低,并伴随着MHC-II high 细胞和CD4 + T细胞。与单独感染小鼠的细胞相比,在不存在IL-4Rα的情况下,sdLN中CD4 + T细胞的数量也有所增加。尽管它们的增殖能力仍然受到损害,但来自4xIL-4RαKO小鼠的sdLN细胞增多与Fas / FasL表达减少相关,导致凋亡减少和细胞死亡,但存活CD4 + T数量增加细胞。这项研究强调了IL-4Rα可以通过诱导IL-10和调节Fas / FasL介导的细胞死亡来调节免疫系统的机制。

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