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首页> 外文期刊>Immunity >Antigen presentation in extracellular matrix: interactions of T cells with dendritic cells are dynamic, short lived, and sequential.
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Antigen presentation in extracellular matrix: interactions of T cells with dendritic cells are dynamic, short lived, and sequential.

机译:细胞外基质中的抗原呈递:T细胞与树突状细胞的相互作用是动态的,短暂的和顺序的。

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摘要

Cognate interactions of naive T cells with antigen-presenting dendritic cells require physical cell-cell contacts leading to signal induction and T cell activation. Using a three-dimensional collagen matrix videomicroscopy model for ovalbumin peptide-specific activation of murine and oxidative mitogenesis of human T cells, we show that T cells maintain vigorous migration upon cognate interactions to DC (dendritic cell), continuously crawl across the DC surface, and rapidly detach (median within 6-12 min). These dynamic and short-lived encounters favor sequential contacts with the same or other DC and trigger calcium influx, upregulation of activation markers, T blast formation, and proliferation. We conclude that a tissue environment supports the accumulation of sequential signals, implicating a numeric or "digital" control mechanism for an ongoing primary immune response.
机译:幼稚T细胞与抗原呈递树突状细胞的同源相互作用需要细胞间的物理接触,从而导致信号诱导和T细胞活化。使用三维胶原蛋白矩阵视频显微镜模型对鼠卵清蛋白肽特异性激活和人类T细胞的氧化有丝分裂进行研究,我们显示,T细胞在同源相互作用与DC(树突状细胞)时保持剧烈迁移,并不断在DC表面上爬行,并迅速分离(中值在6-12分钟之内)。这些动态和短暂的相遇有利于与相同或其他DC的顺序接触,并触发钙内流,激活标记的上调,T胚形成和增殖。我们得出的结论是,组织环境支持连续信号的积累,这牵涉到正在进行的原发性免疫反应的数字或“数字”控制机制。

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