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Characterization of the thymic IL-7 niche in vivo

机译:体内胸腺IL-7生态位的表征

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摘要

The thymus represents the “cradle” for T cell development, with thymic stroma providing multiple soluble and membrane cues to developing thymocytes. Although IL-7 is recognized as an essential factor for thymopoiesis, the “environmental niche” of thymic IL-7 activity remains poorly characterized in vivo. Using bacterial artificial chromosome transgenic mice in which YFP is under control of IL-7 promoter, we identify a subset of thymic epithelial cells (TECs) that co-express YFP and high levels of Il7 transcripts (IL-7hi cells). IL-7hi TECs arise during early fetal development, persist throughout life, and co-express homeostatic chemokines (Ccl19, Ccl25, Cxcl12) and cytokines (Il15) that are critical for normal thymopoiesis. In the adult thymus, IL-7hi cells localize to the cortico-medullary junction and display traits of both cortical and medullary TECs. Interestingly, the frequency of IL-7hi cells decreases with age, suggesting a mechanism for the age-related thymic involution that is associated with declining IL-7 levels. Our temporal-spatial analysis of IL-7-producing cells in the thymus in vivo suggests that thymic IL-7 levels are dynamically regulated under distinct physiological conditions. This IL-7 reporter mouse provides a valuable tool to further dissect the mechanisms that govern thymic IL-7 expression in vivo.
机译:胸腺代表了T细胞发育的“摇篮”,胸腺基质为发育中的胸腺细胞提供了多种可溶性和膜线索。尽管IL-7被认为是胸腺生成的重要因素,但胸腺IL-7活性的“环境生态位”在体内仍然很差。使用其中YFP受IL-7启动子控制的细菌人工染色体转基因小鼠,我们鉴定了共表达YFP和高水平的Il7转录本(IL-7 hi 细胞)。 IL-7 hi TECs在胎儿的早期发育中出现,并在一生中持续存在,并共同表达对正常胸腺生成至关重要的稳态趋化因子(Ccl19,Ccl25,Cxcl12)和细胞因子(Il15)。在成年胸腺中,IL-7 hi 细胞位于皮质-髓质交界处,并显示皮质和髓质TEC的特征。有趣的是,IL-7 hi 细胞的频率会随着年龄的增长而降低,这表明与年龄相关的胸腺退化涉及一种与IL-7水平下降有关的机制。我们对体内胸腺中产生IL-7的细胞进行时空分析表明,胸腺IL-7的水平在不同的生理条件下是动态调节的。该IL-7报告基因小鼠提供了宝贵的工具,可进一步剖析体内控制胸腺IL-7表达的机制。

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