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Both retention and recirculation contribute to long-lived regulatory T-cell accumulation in the thymus

机译:保留和再循环的贡献长寿监管t细胞中积累胸腺

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摘要

Natural Treg cells acquire their lineage-determining transcription factor Foxp3 during development in the thymus and are important in maintaining immunologic tolerance. Here, we analyzed the composition of the thymic Treg-cell pool using RAG2-GFP/FoxP3-RFP dual reporter mice and found that a population of long-lived GFP- Treg cells exists in the thymus. These long-lived Treg cells substantially increased with age, to a point where they represent >90% of the total thymic Treg-cell pool at 6 months of age. In contrast, long-lived conventional T cells remained at ~15% of the total thymic pool at 6 months of age. Consistent with these studies, we noticed that host-derived Treg cells represented a large fraction (~10%) of the total thymic Treg-cell pool in bone marrow chimeras, suggesting that long-lived Treg cells also reside in the thymus of these mice. The pool of long-lived Treg cells in the thymus was sustained by retention of Treg cells in the thymus and by recirculation of peripheral Treg cells back into the thymus. These longlived thymic Treg cells suppressed T-cell proliferation to an equivalent extent to splenic Treg cells. Together, these data demonstrate that long-lived Treg cells accumulate in the thymus by both retention and recirculation.
机译:自然Treg细胞获得他们lineage-determining转录因子Foxp3在胸腺,在开发过程中维持免疫耐受性的重要。在这里,我们分析胸腺的构成使用RAG2-GFP / FoxP3-RFP双重Treg-cell池记者老鼠,发现人口长寿GFP - Treg细胞存在于胸腺。这些长寿大幅Treg细胞随着年龄的增加,到一个地步代表>胸腺Treg-cell池总额的90%在6个月的年龄。传统的T细胞仍在~ 15%胸腺池总在6个月的年龄。通过这些研究,我们发现host-derivedTreg细胞代表了大部分(~ 10%)总胸腺Treg-cell池骨髓嵌合体,这表明长寿Treg细胞也驻留在这些小鼠的胸腺。长寿Treg细胞的胸腺持续的保留Treg细胞胸腺和外围Treg的再循环回胸腺细胞。胸腺Treg细胞抑制t细胞增殖在同等程度上脾Treg细胞。在一起,这些数据表明,长寿Treg细胞在胸腺的积累保留和再循环。

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