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首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >Enhanced renewal of regulatory T cells in relation to CD4+ conventional T lymphocytes in the peripheral compartment
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Enhanced renewal of regulatory T cells in relation to CD4+ conventional T lymphocytes in the peripheral compartment

机译:与周围区室的CD4 +常规T淋巴细胞有关的调节性T细胞更新增强

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CD4(+) Foxp3(+) regulatory T (Treg) cells are necessary for the maintenance of self-tolerance and T-cell homeostasis. This population is kept at stable frequencies in secondary lymphoid organs for the majority of the lifetime, despite permanent thymic emigration or in the face of thymic involution. Continuous competition is expected to occur between recently thymus-emigrated and resident Treg cells (either natural or post-thymically induced). In the present work, we analysed the renewal dynamics of Treg cells compared with CD4(+) Foxp3-conventional T cells (Tconv), using protocols of single or successive T-cell transfers into syngeneic euthymic or lymphopenic (nuu or RAG2(-/-)) mice, respectively. Our results show a higher turnover for Treg cells in the peripheral compartment, compared with Tconv cells, when B cell-sufficient euthymic or nude hosts are studied. This increased renewal within the Treg pool, shown by the greater replacement of resident Treg cells by donor counterparts, correlates with augmented rates of proliferation and is not modified following temporary environmental perturbations induced by inflammatory state or microbiota alterations. Notably, the preferential substitution of Treg lymphocytes was not observed in RAG2(-/-) hosts. We showed that limited B-cell replenishment in the RAG2(-/-) hosts decisively contributed to the altered peripheral T-cell homeostasis. Accordingly, weekly transfers of B cells to RAG2(-/-) hosts rescued the preferential substitution of Treg lymphocytes. Our study discloses a new aspect of T-cell homeostasis that depends on the presence of B lymphocytes to regulate the relative incorporation of recently arrived Treg and Tconv cells in the peripheral compartment.
机译:CD4(+)Foxp3(+)调节性T(Treg)细胞对于维持自我耐受和T细胞稳态是必需的。尽管永久性胸腺迁徙或面对胸腺退化,但在整个生命的大部分时间中,该种群在次要淋巴器官中的频率保持稳定。预期最近迁移的胸腺和居住的Treg细胞(天然或胸腺后诱导)之间会发生持续竞争。在目前的工作中,我们使用CD4(+)Foxp3常规T细胞(Tconv)进行了Treg细胞的更新动力学分析,使用了将单个或连续T细胞转移到同基因的正常或淋巴减少性(nu / nu或RAG2( -/-))小鼠。我们的结果表明,与Tconv细胞相比,当研究B细胞充足的正常或裸露宿主时,Treg细胞的周转率更高。 Treg池中这种更新的增加,表现为供体对应物更多地替代了驻留Treg细胞,与增殖速率增加相关,并且在炎症状态或微生物群改变引起的暂时性环境扰动后并未改变。值得注意的是,在RAG2(-/-)宿主中未观察到Treg淋巴细胞的优先取代。我们显示,RAG2(-/-)宿主中有限的B细胞补给对改变的外周T细胞稳态起了决定性作用。因此,每周将B细胞转移至RAG2(-/-)宿主可拯救Treg淋巴细胞的优先取代。我们的研究揭示了T细胞稳态的一个新方面,它依赖于B淋巴细胞的存在来调节周围细胞中最近到达的Treg和Tconv细胞的相对掺入。

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