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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Anovel function for FOXP3 in humans: Intrinsic regulation of conventional T cells
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Anovel function for FOXP3 in humans: Intrinsic regulation of conventional T cells

机译:FOXP3在人类中的Anovel功能:常规T细胞的内在调节

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The role of forkhead box P3 (FOXP3) is well-established in T-regulatory cells, but the function of transient FOXP3 expression in activated human conventional T (Tconv) cells is unknown. In the present study, we used 2 approaches to determine the role of FOXP3 in human Tconv cells. First, we obtained Tconv clones from a female subject who is hemizygous for a null mutation in FOXP3, allowing the comparison of autologous T-cell clones that do or do not express FOXP3. Second, we knocked down activation-induced FOXP3 in Tconv cells from healthy donors with small interfering RNAagainst FOXP3. We found that FOXP3-deficient Tconv cells proliferate more and produce more cytokines than wild-type Tconv cells and have differential expression of 274 genes. We also investigated the role of FOXP3 in Th1 and Th17 cells and found that the expression of activation-induced FOXP3 was higher and more sustained in Th17 cells compared with Th1 cells. Knocking down FOXP3 expression in Th17 cells significantly increased the production of IFN-?? and decreased the expression of CCR4, but had no effect on IL-17 expression. These data reveal a novel function of FOXP3 in Tconv cells and suggest that expression of this protein is important in the function of multiple CD4+ T-cell lineages.
机译:叉头盒P3(FOXP3)的作用已在T调节细胞中确立,但在活化的人类常规T(Tconv)细胞中瞬时FOXP3表达的功能尚不清楚。在本研究中,我们使用2种方法来确定FOXP3在人类Tconv细胞中的作用。首先,我们从一名女性受试者中获得了Tconv克隆,该受试者对FOXP3中的无效突变是半合子的,从而可以比较表达或不表达FOXP3的自体T细胞克隆。其次,我们敲除健康供体的Tconv细胞中的激活诱导的FOXP3,其中的小干扰RNA对抗FOXP3。我们发现,FOXP3缺陷型Tconv细胞比野生型Tconv细胞增殖更多,产生更多的细胞因子,并且具有274个基因的差异表达。我们还研究了FOXP3在Th1和Th17细胞中的作用,发现与Th1细胞相比,激活诱导的FOXP3在Th17细胞中的表达更高且更持久。抑制Th17细胞中的FOXP3表达可显着增加IFN-γ的产生。降低了CCR4的表达,但对IL-17表达没有影响。这些数据揭示了FOXP3在Tconv细胞中的新功能,并表明该蛋白的表达在多个CD4 + T细胞谱系的功能中很重要。

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