High Thymic Output of Effector CD4+ Cells May Lead to a Treg : T Effector Imbalance in the Periphery in NOD Mice

机译：胸腺高输出的效应CD4 +细胞可能导致NOD小鼠周围的Treg T：T效应失衡。

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Regulatory T cells (Tregs) play a critical role in controlling autoreactive T cells, and quantitative and/or qualitative deficiencies in Tregs are associated with autoimmune diseases, including type 1 diabetes (T1D), in both humans and mice. Both the incidence of T1D and percentages of peripheral Tregs in NOD mice vary considerably between animal facilities. In our animal facility, the incidence of T1D in NOD mice is high at 90-100% and the percentages of peripheral CD4⁺Foxp3⁺ cells in ~9-10-week-old female NOD mice are decreased compared to control (B6) mice shortly before high glucose is first detected (~12 weeks). These data suggest that there is an imbalance between Tregs and potentially pathogenic effector T cells at this age that could have significant impact on disease progression to overt diabetes. The goal of the current study was to investigate mechanisms that play a role in peripheral Treg : T effector cell balance in NOD mice, including differences in persistence/survival, peripheral homeostatic proliferation, and thymic production and output of CD4⁺ T cells. We found no differences in persistence/survival or homeostatic proliferation of either Tregs or effector T cells between NOD and B6 mice. Furthermore, although the percentages and absolute numbers of CD4⁺Foxp3⁺ cells in thymus were not decreased in NOD compared to B6 mice, the percentage of CD4⁺ recent thymic emigrants (RTE) that were Foxp3⁺ was significantly lower in 9-week-old NOD mice. Interestingly, the thymic output of CD4⁺Foxp3⁺ cells was not lower in NOD mice, whereas the thymic output of CD4⁺Foxp3⁻ cells was significantly higher in NOD mice at that age compared to B6 mice. These data suggest that the higher thymic output of CD4⁺Foxp3⁻ T cells contributes, at least in part, to the lower percentages of peripheral CD4⁺Foxp3⁺ Tregs in NOD mice and an imbalance between Tregs and T effector cells that may contribute to the development of full-blown diabetes.

机译：调节性T细胞（Tregs）在控制自身反应性T细胞中起关键作用，并且在人类和小鼠中，Tregs的定量和/或定性缺陷均与自身免疫性疾病（包括1型糖尿病（T1D））相关。在不同的动物设施之间，NOD小鼠中T1D的发生率和周围Treg的百分比都存在很大差异。在我们的动物设施中，NOD小鼠中T1D的发生率高达90-100％，并且在大约9-10-周内其外周CD4 ^{+ Foxp3 ^{+ 细胞的百分比在首次检测到高血糖之前（约12周），与对照组（B6）小鼠相比，雌性NOD小鼠的年龄减少了。这些数据表明，在这个年龄的Treg和潜在致病性效应T细胞之间存在失衡，这可能对疾病向明显的糖尿病的发展产生重大影响。本研究的目的是研究在NOD小鼠外周Treg：T效应细胞平衡中起作用的机制，包括持久性/存活率，外周稳态增殖以及胸腺CD4 ^{+产生和输出的差异 T细胞。我们发现在NOD和B6小鼠之间，Tregs或效应T细胞的持久性/存活性或体内稳态增殖没有差异。此外，尽管与B6小鼠相比，NOD小鼠胸腺中CD4 ^{+ Foxp3 ^{+ 细胞的百分比和绝对数量没有减少，但CD4 ^{+ 9周龄的NOD小鼠中的Foxp3 ^{+ 胸腺最近迁出者（RTE）明显降低。有趣的是，在NOD小鼠中CD4 ^{+ Foxp3 ^{+ 细胞的胸腺输出并不降低，而CD4 ^{+ Foxp3 ^{的胸腺输出与B6小鼠相比，在那个年龄的NOD小鼠中− 细胞明显更高。这些数据表明，CD4 ^{+ Foxp3 ^{- T细胞的胸腺输出较高，至少部分地有助于降低外周CD4 ^{+ Foxp3 ^{+ Tregs以及Tregs和T效应细胞之间的失衡，可能导致成熟的糖尿病的发展。}}}}}}}}}}}}}}}

著录项

期刊名称 Clinical and Developmental Immunology
作者
Yuan Zhao; Pascale Alard; Michele M. Kosiewicz;
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年(卷),期 2019(2019),-1
年度 2019
页码 8785263
总页数 14
原文格式 PDF
正文语种
中图分类免疫学;
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专利

1. High Thymic Output of Effector CD4+ Cells May Lead to a Treg?:?T Effector Imbalance in the Periphery in NOD Mice [J] . Yuan Zhao, Pascale Alard, Michele M. Kosiewicz Journal of immunology research. . 2019,第1期

机译：效应CD4 +细胞的高胸腺输出可能导致Treg？：ΔTα在NOD小鼠中的周边效应不平衡
2. Function of CD4+,CD25+ Treg cells in MRL/lpr mice is compromised by intrinsic defects in antigen-presenting cells and effector T cells. [J] . Parietti V, Monneaux F, Decossas M, Arthritis and Rheumatism . 2008,第6期

机译：MRL / lpr小鼠中CD4 +，CD25 + Treg细胞的功能受到抗原呈递细胞和效应T细胞内在缺陷的损害。
3. Deletion of Fibrinogen-like Protein 2 (FGL-2), a Novel CD4+ CD25+ Treg Effector Molecule, Leads to Improved Control of Echinococcus multilocularis Infection in Mice [J] . Junhua Wang, Dominique A. Vuitton, Norbert Müller, PLOS Neglected Tropical Diseases . 2015,第5期

机译：缺失纤维蛋白原蛋白2（FGL-2），一种新的CD4 + CD25 + Treg效应分子，导致小鼠呼吸膜球菌多层感染的改善
4. Strategies for overcoming the adverse effects of imbalances in the second order reactions in valve regulated lead acid cells [C] . Brecht, W.B. . 2002

机译：克服阀控铅酸电池中二级反应不平衡的不利影响的策略
5. TCR dependent thymic Treg differentiation and Th17 cells in experimental autoimmune encephalomyelitis. [D] . Leung, Monica W. L. 2010

机译：实验性自身免疫性脑脊髓炎中，TCR依赖性胸腺Treg分化和Th17细胞。
6. The presence and preferential activation of Tregs diminishes adoptive transfer of autoimmune diabetes by polyclonal NOD T cell effectors into NSG versus NOD-scid mice [O] . Maximiliano Presa, Yi-Guang Chen, Alexandra E. Grier, -1

机译：Tregs的存在和优先激活减少了多克隆NOD T细胞效应子向NSG和NOD-scid小鼠体内自身免疫性糖尿病的过继转移
7. Selective infection of CD4+ effector memory T lymphocytes leads to preferential depletion of memory T lymphocytes in R5 HIV-1-infected humanized NOD/SCID/IL-2Rγnull mice [O] . Nie Chuanyi, Sato Kei, Misawa Naoko, 2009

机译：CD4 +效应记忆T淋巴细胞的选择性感染导致R5 HIV-1感染的人源化NOD / SCID /IL-2Rγnull小鼠的记忆T淋巴细胞优先消耗

High Thymic Output of Effector CD4+ Cells May Lead to a Treg : T Effector Imbalance in the Periphery in NOD Mice

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