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体外扩增可改善CD4+CD25+调节性T细胞的体内调节作用。

In vitro expansion improves in vivo regulation by CD4+CD25+ regulatory T cells.

作者信息

Chai Jian-Guo, Coe David, Chen Daxin, Simpson Elizabeth, Dyson Julian, Scott Diane

机构信息

Cancer Immunotherapy Group, Department of Immunology, Imperial College London, UK.

出版信息

J Immunol. 2008 Jan 15;180(2):858-69. doi: 10.4049/jimmunol.180.2.858.

DOI:10.4049/jimmunol.180.2.858
PMID:18178825
Abstract

CD4+CD25+ T regulatory cells (Tregs) can actively suppress immune responses and thus have substantial therapeutical potential. Clinical application is, however, frustrated by their scarcity, anergic status, and lack of defined specificity. We found that a single injection of a small number of expanded but not fresh HY-specific Tregs protected syngeneic male skin grafts from rejection by immune-competent recipients. The expanded Tregs were predominantly located in the grafts and graft-draining lymph nodes. In vitro expanded Tregs displayed a phenotype of CD25highCD4lowFoxp3+CTLA4+, and also up-regulated IL10 and TGFbeta while down-regulating IFN-gamma, GM-CSF, IL5, and TNF-alpha production. Furthermore, expanded Tregs appeared to express a reduced level of Foxp3, which could be prevented by adding TGFbeta to the culture, and they also tended to lose Foxp3 following the repeated stimulation. Finally, a proportion of expanded HY-specific Tregs secreted IL2 in response to their cognate peptide, and this finding could be confirmed using Tregs from Foxp3GFP reporter mice. We not only demonstrated that expanded Tregs are superior to fresh Tregs in suppressing T cell responses against alloantigens, but also revealed some novel immunobiological properties of expended Tregs which are very instructive for modifying current Treg expansion procedures.

摘要

CD4+CD25+调节性T细胞(Tregs)能够积极抑制免疫反应,因此具有巨大的治疗潜力。然而,其稀缺性、无反应状态以及缺乏明确的特异性阻碍了它们在临床上的应用。我们发现,单次注射少量经扩增而非新鲜的HY特异性Tregs可保护同基因雄性皮肤移植物不被免疫活性受体排斥。扩增后的Tregs主要位于移植物和引流移植物的淋巴结中。体外扩增的Tregs表现出CD25高CD4低Foxp3+CTLA4+的表型,同时上调IL10和TGFβ,而下调IFN-γ、GM-CSF、IL5和TNF-α的产生。此外,扩增后的Tregs似乎表达较低水平的Foxp3,在培养中添加TGFβ可防止这种情况,并且在反复刺激后它们也倾向于失去Foxp3。最后,一部分扩增后的HY特异性Tregs在接触其同源肽后分泌IL2,这一发现可以用来自Foxp3GFP报告基因小鼠的Tregs得到证实。我们不仅证明了扩增后的Tregs在抑制针对同种异体抗原的T细胞反应方面优于新鲜Tregs,还揭示了扩增后Tregs的一些新的免疫生物学特性,这对于改进当前的Treg扩增程序具有重要的指导意义。

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