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Helios + + and Helios ? ? Treg subpopulations are phenotypically and functionally distinct and express dissimilar TCR repertoires

机译:赫利俄斯+ +和赫利俄斯?表型和功能不同表达不同的TCR体验

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摘要

Abstract The transcription factor Helios is expressed in a large subset of Foxp3 + Tregs. We previously proposed that Helios is a marker of thymic derived Treg (tTreg), while Helios ? Treg were induced from Foxp3 ? T conventional (Tconv) cells in the periphery (pTreg). To compare the two Treg subpopulations, we generated Helios‐GFP reporter mice and crossed them to Foxp3‐RFP reporter mice. The Helios + Treg population expressed a more activated phenotype, had a slightly higher suppressive capacity in vitro and expressed a more highly demethylated TSDR but were equivalent in their ability to suppress inflammatory bowel disease in vivo. However, Helios + Treg more effectively inhibited the proliferation of activated, autoreactive splenocytes from scurfy mice. When Helios + and Helios ? Treg were transferred to lymphoreplete mice, both populations maintained comparable Foxp3 expression, but Foxp3 expression was less stable in Helios ? Treg when transferred to lymphopenic mice. Gene expression profiling demonstrated a large number of differentially expressed genes and showed that Helios ? Treg expressed certain genes normally expressed in CD4 + Foxp3 ? T?cells. TCR repertoire analysis indicated very little overlap between Helios + and Helios ? Treg. Thus, Helios + and Helios ? Treg subpopulations are phenotypically and functionally distinct and express dissimilar TCR repertoires.
机译:摘要转录因子赫利俄斯表示在一个大的子集Foxp3 +亚群。之前提出,赫利俄斯的标志胸腺派生Treg (tTreg),赫利俄斯?从Foxp3诱导?细胞外围(pTreg)。两个Treg亚种群,我们生成的Helios GFP记者老鼠和交叉Foxp3 RFP应承担的记者老鼠。表达了更多的激活表型,在体外和稍高的抑制能力表达了高度脱甲基TSDR但是相当于他们的抑制能力吗炎症性肠病体内。赫利俄斯+ Treg更有效地抑制了扩散激活,autoreactive从皮屑小鼠脾细胞。赫利俄斯?老鼠,两个种群保持可比Foxp3的表达,但Foxp3表达更少在赫利俄斯稳定吗?lymphopenic老鼠。展示了大量的不同表达基因和显示,赫利俄斯?通常表示某些基因表达CD4+ Foxp3 ?表示很少重叠Helios +赫利俄斯?Treg种群在表型和功能不同,表达不同的细胞repertoires。

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