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Tissue adaptation of regulatory T cells in adipose tissue

机译:脂肪组织中调节性T细胞的组织适应

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Abstract Foxp3+ regulatory T (Treg) cells critically suppress over‐activated immune responses and therefore maintain immune homeostasis. Adipose tissue‐resident Treg (AT Treg) cells are known for modulating immunity and metabolism in adipose tissue microenvironment through various physiological signals, as well as their heterogeneous subsets, which potentially play disparate roles in aging and obesity. Recent single‐cell studies of Treg cells have revealed specialized trajectories of their tissue adaptation and development in lymphoid tissues and at barrier sites. Here, we reviewed a T Cell Receptor (TCR)‐primed environmental cue‐boosted model of adipose Treg cells’ tissue adaptation, especially in response to IL‐33, IFN‐α, insulin, and androgen signals, which trigger sophisticated transcriptional cascades and ultimately establish unique transcriptional modules in adipose Treg cell subsets. In addition, we further discuss potential therapeutic strategies against aging and obesity by blocking detrimental environmental cues, strengthening the functions of specific AT Treg subsets?and modifying the communications between AT Treg subsets and adipocytes.
机译:抽象Foxp3 +调节性T (Treg)细胞严重抑制/激活免疫反应,因此维持免疫体内平衡。Treg)调节免疫和细胞代谢脂肪组织微环境通过各种生理信号,以及他们的异构子集,这可能扮演不同的角色在衰老和肥胖。单量Treg细胞显示细胞的研究专业组织的轨迹淋巴组织的适应和发展网站和障碍。受体(TCR)应承担的环境线索量增加脂肪Treg细胞模型的组织改编,尤其是在应对IL高33干扰素α,应承担的胰岛素,雄激素信号,触发复杂转录级联,最终建立在脂肪Treg独特的转录模块细胞的子集。防止衰老的潜在的治疗策略和肥胖通过阻断有害环境线索,加强特定的功能Treg子集?在Treg子集和脂肪细胞之间的关系。

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