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移植中的调节性 T 细胞:细胞外三磷酸腺苷代谢通过 CD39 是否起关键作用?

Regulatory T cells in transplantation: does extracellular adenosine triphosphate metabolism through CD39 play a crucial role?

机构信息

Renal Medicine Department, Singapore General Hospital, Singapore.

出版信息

Transplant Rev (Orlando). 2010 Apr;24(2):52-66. doi: 10.1016/j.trre.2010.01.002. Epub 2010 Feb 11.

DOI:10.1016/j.trre.2010.01.002
PMID:20153159
Abstract

Despite tremendous improvements in short-term renal allograft survival, many patients still have chronic rejection or side effects of nonspecific immunosuppression. The discovery of Foxp3(+) regulatory T cells (Tregs) has revolutionized the concepts in immunoregulation and offers perspectives for overcoming rejection. Recently, a subset of Foxp3(+)CD39(+) effector/memory-like Tregs (T(REM)) was identified. The role of CD39(+) Tregs in immunoregulation is supported by the occurrence of alopecia areata and experimental autoimmune encephalomyelitis in CD39-deficient mice and by the failure of CD39(-) Tregs to suppress contact hypersensitivity. In humans, CD39 polymorphisms have been associated with diabetes and nephropathy, and multiple sclerosis patients have reduced numbers of blood CD39(+) Tregs. Preliminary experiments in a murine transplantation model showed that CD39(+) Tregs can determine allograft outcome. CD39 degrades the extracellular adenosine triphosphate (ATP) released during tissue injury, which otherwise would trigger inflammation. Currently, our groups are assessing the role of CD39(+) Tregs and extracellular ATP metabolism in clinical transplantation and whether tolerogenic Treg profiles possess immunopredictive value, envisioning the development of clinical trials using CD39(+) Treg-based vaccination for autoimmunity or transplantation. This is a comprehensive review on the fundamentals of Treg biology, the potential role of ATP metabolism in immunoregulation, and the potential use of Treg-based immunotherapy in transplantation.

摘要

尽管短期肾移植存活率有了显著提高,但许多患者仍存在慢性排斥反应或非特异性免疫抑制的副作用。Foxp3(+)调节性 T 细胞(Tregs)的发现彻底改变了免疫调节的概念,并为克服排斥反应提供了新的思路。最近,人们发现了 Foxp3(+)CD39(+)效应/记忆样 Tregs(T(REM))亚群。CD39(+)Tregs 在免疫调节中的作用得到了以下事实的支持:CD39 缺陷小鼠会发生斑秃和实验性自身免疫性脑脊髓炎,而 CD39(-)Tregs 无法抑制接触性超敏反应。在人类中,CD39 多态性与糖尿病和肾病有关,多发性硬化症患者的血液 CD39(+)Tregs 数量减少。在小鼠移植模型的初步实验中,发现 CD39(+)Tregs 可以决定移植物的结局。CD39 可降解组织损伤时释放的细胞外三磷酸腺苷(ATP),否则该物质会引发炎症。目前,我们的团队正在评估 CD39(+)Tregs 和细胞外 ATP 代谢在临床移植中的作用,以及耐受型 Treg 表型是否具有免疫预测价值,设想开发使用 CD39(+)Treg 为基础的疫苗进行自身免疫或移植的临床试验。本文对 Treg 生物学的基础、ATP 代谢在免疫调节中的潜在作用以及基于 Treg 的免疫疗法在移植中的潜在应用进行了全面的综述。

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