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首页> 外文期刊>The journal of immunology >Local “On-Demand” Generation and Function of Antigen-Specific Foxp3+ Regulatory T Cells
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Local “On-Demand” Generation and Function of Antigen-Specific Foxp3+ Regulatory T Cells

机译:抗原特异性Foxp3 +调节性T细胞的局部“按需”生成和功能

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摘要

Extrathymically derived regulatory T cells (iTregs) protect against autoimmunity to tissue-specific Ags. However, whether Ag-specific iTreg generation and function is limited to secondary lymphoid tissue or whether it can occur within the tissue-specific local environment of the cognate Ag remains unresolved. Mice expressing β-galactosidase (βgal) on a retina-specific promoter (βgal mice) in conjunction with mice expressing GFP and diphtheria toxin (DTx) receptor (DTR) under control of the Foxp3 promoter, and βgal-specific TCR transgenic (BG2) mice were used to examine this question. Local depletion (ocular DTx), but not systemic depletion (i.p. DTx), of βgal-specific iTregs enhanced experimental autoimmune uveoretinitis induced by activated βgal-specific effector T cells. Injections of small amounts of βgal into the anterior chamber of the eye produced similar numbers of βgal-specific iTregs in the retina whether the mouse was depleted of pre-existing, circulating Tregs. Taken together, these results suggest that protection from tissue-specific autoimmunity depends on the function of local Ag-specific iTregs and that the retina is capable of local, “on-demand” iTreg generation that is independent of circulating Tregs.
机译:胸腺外来源的调节性T细胞(iTregs)可防止针对组织特异性Ag的自身免疫。但是,是否仍需要进一步研究Ag特异的iTreg的生成和功能是否局限于继发性淋巴样组织或是否可以在同源Ag的组织特异的局部环境中发生。在视网膜特异性启动子(βgal小鼠)上表达β-半乳糖苷酶(βgal)的小鼠与在Foxp3启动子控制下表达GFP和白喉毒素(DTx)受体(DTR)的小鼠以及βgal特异性TCR转基因(BG2)小鼠被用来检验这个问题。 βgal特异性iTreg的局部耗竭(眼部DTx)而非全身耗竭(i.p. DTx)增强了激活的βgal特异性效应T细胞诱导的实验性自身免疫性葡萄膜视网膜炎。不论老鼠是否已经耗尽循环中的Treg,向眼睛前房注射少量βgal都会在视网膜中产生相似数量的βgal特异性iTreg。综上所述,这些结果表明,针对组织特异性自身免疫的保护取决于局部Ag特异性iTreg的功能,并且视网膜能够产生独立于循环Treg的局部“按需” iTreg生成。

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