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Tentative T Cells: Memory Cells Are Quick to Respond but Slow to Divide

机译:暂定T细胞:记忆细胞反应迅速但分裂缓慢

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摘要

T cell memory is a cornerstone of protective immunity, and is the key element in successful vaccination. Upon encountering the relevant pathogen, memory T cells are thought to initiate cell division much more rapidly than their naïve counterparts, and this is thought to confer a significant biological advantage upon an immune host. Here, we use traceable TCR-transgenic T cells to evaluate this proposed characteristic in CD4+ and CD8+ memory T cells. We find that, even in the presence of abundant antigen that was sufficient to induce in vivo IFNγ production by memory T cells, both memory and naïve T cells show an extended, and indistinguishable, delay in the onset of proliferation. Although memory cells can detect, and respond to, virus infection within a few hours, their proliferation did not begin until ∼3 days after infection, and occurred simultaneously in all anatomical compartments. Thereafter, cell division was extraordinarily rapid for both naïve and memory cells, with the latter showing a somewhat accelerated accumulation. We propose that, by permitting memory T cells to rapidly exert their effector functions while delaying the onset of their proliferation, evolution has provided a safeguard that balances the risk of infection against the consequences of severe T cell–mediated immunopathology.
机译:T细胞记忆是保护性免疫的基石,是成功接种疫苗的关键因素。遇到相关病原体后,记忆T细胞被认为比其幼稚的T细胞更快地启动细胞分裂,这被认为为免疫宿主带来了重要的生物学优势。在这里,我们使用可追踪的TCR转基因T细胞来评估CD4 + 和CD8 + 记忆T细胞中的拟议特征。我们发现,即使存在足够的抗原,足以诱导记忆T细胞在体内产生IFNγ,记忆和幼稚T细胞在增殖开始时均显示出延长且难以区分的延迟。尽管记忆细胞可以在几小时内检测到病毒并对其作出反应,但它们的增殖直到感染后约三天才开始,并在所有解剖室同时发生。此后,幼稚和记忆细胞的细胞分裂异常迅速,后者显示出一定程度的加速积累。我们提出,通过允许记忆性T细胞在延迟其增殖开始时迅速发挥其效应子功能,进化提供了一种保护措施,可以平衡感染风险与严重T细胞介导的免疫病理后果之间的平衡。

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