寡核苷酸在体外扩增过程中稳定表达 Helios 的 Foxp3+ 人类 T 调节细胞。
Oligodeoxynucleotides stabilize Helios-expressing Foxp3+ human T regulatory cells during in vitro expansion.
机构信息
Laboratory of Immunology, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892, USA.
出版信息
Blood. 2012 Mar 22;119(12):2810-8. doi: 10.1182/blood-2011-09-377895. Epub 2012 Jan 31.
Abstract
Foxp3(+) regulatory T cells (Tregs) maintain self-tolerance and adoptive therapy, and using Foxp3(+) Tregs has been proposed as treatment for autoimmune diseases. The clinical use of Tregs will require large numbers of cells and methods for in vitro expansion of Tregs are being developed. Foxp3(+) Tregs can be divided into 2 subpopulations based on expression of the transcription factor, Helios. Foxp3(+)Helios(+) Tregs (70%) are thymic-derived, whereas Foxp3(+)Helios(-) Tregs (30%) are induced in the periphery. Foxp3(+)Helios(+) Tregs differ from Foxp3(+)Helios(-) Tregs in terms of epigenetic changes at the Foxp3 locus, their capacity to produce effector cytokines, and their stability of Foxp3 expression on days to weeks of expansion in vitro. Addition of a 25 mer DNA oligonucleotide of random composition for a short period during the expansion of Foxp3(+) Tregs in vitro results in prolonged stabilization of the Foxp3(+)Helios(+) subpopulation and yields an optimal population for use in cellular biotherapy.
摘要
Foxp3(+)调节性 T 细胞 (Tregs) 维持自身耐受和过继治疗,并且使用 Foxp3(+)Tregs 已被提议作为治疗自身免疫性疾病的方法。Tregs 的临床应用将需要大量的细胞,并且正在开发 Tregs 的体外扩增方法。根据转录因子 Helios 的表达,Foxp3(+)Tregs 可分为 2 个亚群。Foxp3(+)Helios(+)Tregs(70%)是胸腺来源的,而 Foxp3(+)Helios(-)Tregs(30%)是在外周诱导的。Foxp3(+)Helios(+)Tregs 在 Foxp3 基因座的表观遗传变化、产生效应细胞因子的能力以及体外扩增数天至数周时 Foxp3 表达的稳定性方面与 Foxp3(+)Helios(-)Tregs 不同。在体外扩增 Foxp3(+)Tregs 的过程中,短时间内添加一段由随机组成的 25 个碱基对的 DNA 寡核苷酸,可延长 Foxp3(+)Helios(+)亚群的稳定,并产生用于细胞生物治疗的最佳群体。
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Massive ex vivo expansion of human natural regulatory T cells (T(regs)) with minimal loss of in vivo functional activity.大量扩增人源天然调节性 T 细胞(Tregs),同时最小化体内功能活性损失。
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