EGR2 is elevated and positively regulates inflammatory IFNγ production in lupus CD4 + T cells

Rujuan Dai; Bettina Heid; Xiguang Xu; Hehuang Xie; Christopher M. Reilly; S. Ansar Ahmed

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EGR2 is elevated and positively regulates inflammatory IFNγ production in lupus CD4 + T cells

机译：EGR2升高，并积极地调节狼疮CD4 + T细胞中的炎症IFNγ产生

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Recent studies have shown that early growth response 2 (EGR2) is highly induced in activated T cells and regulates T cell functions. In normal C57BL/6 (B6) mice, deletion of EGR2 in lymphocytes results in the development of lupus-like systemic autoimmune disease, which implies indirectly an autoimmune protective role of EGR2. Conversely, increased EGR2 gene expression is suggested to link with high risk of human lupus. In the present studies we sought to clarify the expression and inflammation regulatory role of EGR2 in murine lupus T cells directly. We performed RT-qPCR analysis and found a significant increase of EGR2 mRNA expression in human lupus PBMCs and in CD4+ T cells from three different murine lupus models including MRL-lpr, B6-lpr, and B6.sle123 mice at diseased stage when compared to age-matched control MRL or B6 mice. By performing intracellular flow cytometry analysis, we found that EGR2 protein expression was significantly increased in resting lupus (either MRL-lpr or B6.sle123) CD4+ T cells when compared to CD4+ T cells from their respective non-autoimmune controls. However, there was no difference of EGR2 protein expression in anti-CD3 and anti-CD28 stimulated control and lupus CD4+ T cells since there was a stronger induction of EGR2 in activated control CD4+ T cells. EGR2 expression was significantly increased in MRL-lpr mice at an age when lupus is manifested. To understand further the function of elevated EGR2 in lupus CD4+ T cells, we inhibited EGR2 with a specific siRNA in vitro in splenocytes from MRL-lpr and control MRL mice at 15?weeks-of-age. We found that EGR2 inhibition significantly reduced IFNγ production in PMA and ionomycin activated MRL-lpr lupus CD4+ T cells, but not control MRL CD4+ T cells. We also found that inhibition of EGR2 in vitro suppressed the Th1 differentiation in both MRL and MRL-lpr na?ve CD4+ T cells. EGR2 is highly upregulated in human and murine lupus cells. Our in vitro data suggest a positive role of EGR2 in the regulation of Th1 differentiation and IFNγ production in lupus effector CD4+ T cells.

机译：最近的研究表明，早期生长响应2（EGR2）在活性T细胞中高度诱导并调节T细胞功能。在正常的C57BL / 6（B6）小鼠中，淋巴细胞中EGR2的缺失导致狼疮的系统自身免疫疾病的发展，这意味着EGR2的自身免疫保护作用。相反，建议增加EGR2基因表达，以与人狼疮的高风险联系起来。在本研究中，我们试图阐明EGR2在鼠狼疮T细胞中EGR2在鼠狼T细胞中的表达和炎症调节作用。我们进行了RT-QPCR分析，发现人狼疮PBMC中的EGR2 mRNA表达和来自三种不同鼠狼疮模型的CD4 + T细胞的显着增加，包括MRL-LPR，B6-LPR和B6.SLE123小鼠在患病阶段年龄匹配的对照MRL或B6小鼠。通过进行细胞内流式细胞术分析，我们发现与它们各自的非自身免疫对照相比，在静止的狼疮（MRL-LPR或B6.SLE123）CD4 + T细胞中显着增加EGR2蛋白表达。然而，在抗CD3和抗CD28刺激的对照和狼疮CD4 + T细胞中没有差异差异，因为在活化的对照CD4 + T细胞中较强诱导EGR2。当狼疮表现出时，MRL-LPR小鼠在MRL-LPR小鼠中显着增加。为了进一步了解狼疮CD4 + T细胞中升高的EGR2的功能，我们抑制了来自MRL-LPR的脾细胞的特异性siRNA的EGR2，并在15-岁的时间为15？岁的时间。我们发现EGR2抑制显着降低了PMA和离子霉素活化MRL-LPR狼疮CD4 + T细胞的IFNγ产生，但不控制MRL CD4 + T细胞。我们还发现抑制EGR2在体外抑制MRL和MRL-LPR Naαva-Ve CD4 + T细胞中的Th1分化。 EGR2在人和鼠狼疮细胞中高度上调。我们的体外数据表明EGR2在卢布效应器CD4 + T细胞中Th1分化和IFNγ产生的调节中的积极作用。

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《BMC Immunology》 |2020年第1期|共14页
作者
Rujuan Dai; Bettina Heid; Xiguang Xu; Hehuang Xie; Christopher M. Reilly; S. Ansar Ahmed;
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EGR2LupusInflammationIFNγTh1;

机译：egr2lupusinflammationifnγth1.;

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专利

1. Factors involved in the differentiation of TGF-beta-producing cells from naive CD4+ T cells: IL-4 and IFN-gamma have opposing effects, while TGF-beta positively regulates its own production. [J] . Seder RA, Marth T, Sieve MC, The Journal of Immunology: Official Journal of the American Association of Immunologists . 1998,第12期

机译：涉及从原始CD4 + T细胞分化TGF-β产生细胞的因素：IL-4和IFN-γ具有相反的作用，而TGF-β积极调节其自身的产生。
2. CD40 ligand/CD40 stimulation regulates the production of IFN-gamma from human peripheral blood mononuclear cells in an IL-12- and/or CD28-dependent manner. [J] . McDyer JF, Goletz TJ, Thomas E, The Journal of Immunology: Official Journal of the American Association of Immunologists . 1998,第4期

机译：CD40配体/ CD40刺激以IL-12和/或CD28依赖性方式调节人外周血单核细胞产生IFN-γ。
3. CD40 Ligand/CD40 Stimulation Regulates the Production of IFN-γ from Human Peripheral Blood Mononuclear Cells in an IL-12- and/or CD28-Dependent Manner [J] . John F. McDyer, Theresa J. Goletz, Elaine Thomas, The journal of immunology . 1998,第4期

机译：CD40配体/ CD40刺激以IL-12和/或CD28依赖性方式调节人外周血单核细胞产生IFN-γ。
4. ALGINIC ACID OLIGOSACCHARIDE UP-REGULATES IFN-γ PRODUCTION BY LYMPH NODE CELLS [C] . Tadashi Yoshida, Aki Hirano, Hanae Wada, Annual Meeting of the Japanese Association for Animal Cell Technology . 2003

机译：含有淋巴结细胞的藻酸寡糖升高IFN-γ产生
5. Autoimmune kidney damage correlates with autoantibody specificity and inflammatory mononuclear cell phenotype in the CD45 mutant mouse model of lupus [D] . Hai, Si-Han 2015

机译：狼疮CD45突变小鼠模型中，自身免疫性肾脏损伤与自身抗体特异性和炎性单核细胞表型相关
6. EGR2 is elevated and positively regulates inflammatory IFNγ production in lupus CD4+ T cells [O] . Rujuan Dai, Bettina Heid, Xiguang Xu, 2020

机译：EGR2升高并积极地调节狼疮CD4 + T细胞中的炎症IFNγ产生
7. CD4+ T cells induced by virus-like particles expressing a major T cell epitope down-regulate IL-5 production in an ongoing immune response to Der p 1 independently of IFN-γ production [O] . Sandra Hirschberg, Guy T. Layton, Stephen J. Harris, 1999

机译：由病毒样颗粒诱导的CD4 + T细胞，其表达主要T细胞表位下调IL-5在持续的免疫应答中产生，以DER P 1独立于IFN-γ生产

EGR2 is elevated and positively regulates inflammatory IFNγ production in lupus CD4 + T cells

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