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Differential Cytokine Utilization and Tissue Tropism Results in Distinct Repopulation Kinetics of Naïve vs. Memory T Cells in Mice

机译:差异细胞因子的利用和组织趋向导致幼稚与记忆T细胞在小鼠中的独特的再填充动力学

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摘要

Naïve and memory T cells co-exist in the peripheral T cell pool, but the cellular mechanisms that maintain the balance and homeostasis of these two populations remain mostly unclear. To address this question, here, we assessed homeostatic proliferation and repopulation kinetics of adoptively transferred naïve and memory T cells in lymphopenic host mice. We identified distinct kinetics of proliferation and tissue-distribution between naïve and memory donor T cells, which resulted in the occupancy of the peripheral T cell pool by mostly naïve-origin T cells in short term (<1 week), but, in a dramatic reversal, by mostly memory-origin T cells in long term (>4 weeks). To explain this finding, we assessed utilization of the homeostatic cytokines IL-7 and IL-15 by naïve and memory T cells. We found different efficiencies of IL-7 signaling between naïve and memory T cells, where memory T cells expressed larger amounts of IL-7Rα but were significantly less potent in activation of STAT5 that is downstream of IL-7 signaling. Nonetheless, memory T cells were superior in long-term repopulation of the peripheral T cell pool, presumably, because they preferentially migrated into non-lymphoid tissues upon adoptive transfer and additionally utilized tissue IL-15 for rapid expansion. Consequently, co-utilization of IL-7 and IL-15 provides memory T cells a long-term survival advantage. We consider this mechanism important, as it permits the memory T cell population to be maintained in face of constant influx of naïve T cells to the peripheral T cell pool and under competing conditions for survival cytokines.
机译:幼稚和记忆性T细胞共存于外周T细胞池中,但是维持这两个群体平衡和体内稳态的细胞机制仍不清楚。为了解决这个问题,在这里,我们评估了在淋巴细胞减少的宿主小鼠中过继转移的幼稚和记忆T细胞的稳态增殖和种群动力学。我们确定了幼稚和记忆供体T细胞之间增殖和组织分布的独特动力学,这导致短期(<1周)内大多数幼稚T细胞占据了外周T细胞池,但是在长期(> 4周)内,大部分是记忆起源的T细胞发生逆转。为了解释这一发现,我们评估了幼稚和记忆T细胞对稳态细胞因子IL-7和IL-15的利用。我们发现幼稚和记忆T细胞之间的IL-7信号传导效率不同,其中记忆T细胞表达大量的IL-7Rα,但在激活IL-7信号下游的STAT5方面的效力明显较低。尽管如此,据推测,记忆T细胞在外周T细胞库的长期再繁殖方面是优越的,推测是因为它们在过继转移时优先迁移到非淋巴组织中,并另外利用组织IL-15进行快速扩增。因此,IL-7和IL-15的共同利用为记忆T细胞提供了长期生存优势。我们认为这种机制很重要,因为它允许面对幼稚T细胞不断涌入外周T细胞池并在生存细胞因子竞争的条件下保持记忆T细胞种群。

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