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首页> 外文期刊>Scandinavian journal of immunology. >Nicotine Exposure Alters the mRNA Expression of Notch Ligands in Dendritic Cells and Their Response to Th1-/Th2-Promoting Stimuli
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Nicotine Exposure Alters the mRNA Expression of Notch Ligands in Dendritic Cells and Their Response to Th1-/Th2-Promoting Stimuli

机译:尼古丁暴露改变了树突状细胞中Notch配体的mRNA表达及其对Th1- / Th2-刺激的响应

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摘要

Dendritic cells (DCs) utilize polarizing signals to instruct the differentiation of T helper (Th) cells into Th1 and Th2 effector cells: antigen-specific signal 1', costimulatory signal 2' and polarizing cytokines signal 3'. Accumulating evidence suggests the involvement of an additional signal, the Notch signalling pathway. We reported that in response to Th1-promoting stimuli, both mouse and human DCs generated in the presence of the immune modulator nicotine (nicDCs) fail to support the development of effector memory Th1 cells. However, in response to Th2-promoting stimuli, these nicDCs preferentially support the differentiation of antigen-specific IL-4-producing Th2 effector cells. Here, we show that when compared to their control counterparts, immature mouse and human nicDCs display higher levels of the Notch ligands D1, D4 and J2 mRNA expression. In response to Th1- and Th2-promoting stimuli, mouse nicDCs display higher levels of the Notch ligands D1, D4 and J2, while human nicDCs show higher levels of D1, D4 and J1 mRNA expression. Furthermore, both stimulated mouse and human nicDCs express higher CD86 to CD80 ratio and produce lower amount of IL-12. Collectively, our data suggest that these changes in addition to an increase in Jagged expression correlate with the ability of nicDCs to modulate the Th1/Th2 balance in favour of Th2 generation.
机译:树突状细胞(DC)利用极化信号指示T辅助(Th)细胞分化为Th1和Th2效应细胞:抗原特异性信号1',共刺激信号2'和极化细胞因子信号3'。越来越多的证据表明,Notch信号通路参与了另一个信号。我们报告说,响应于Th1促进刺激,在免疫调节剂尼古丁(nicDCs)的存在下产生的小鼠和人类DC都无法支持效应记忆Th1细胞的发展。但是,响应于Th2刺激,这些nicDCs优先支持分化产生抗原的IL-4的Th2效应细胞。在这里,我们表明,与对照组相比,未成熟的小鼠和人nicDCs显示出更高水平的Notch配体D1,D4和J2 mRNA表达。响应Th1和Th2促进刺激,小鼠nicDCs显示出更高水平的Notch配体D1,D4和J2,而人nicDCs显示出更高水平的D1,D4和J1 mRNA表达。此外,受刺激的小鼠和人nicDC均表达较高的CD86与CD80比率,并产生较低量的IL-12。总体而言,我们的数据表明,除了锯齿状表达的增加以外,这些变化还与nicDCs调节Th1 / Th2平衡以支持Th2产生的能力有关。

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