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Peripheral differentiation patterns of human T cells

机译:外围分化的人类T模式细胞

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Abstract Long‐term T‐cell memory is dependent on the maintenance of memory T cells in the lymphoid tissues, and at the surface interfaces that provide entry routes for pathogens. However, much of the current information on human T‐cell memory is based on analyzing circulating T cells. Here, we have studied the distribution and age‐related changes of memory T‐cell subsets in samples from blood, mesenteric LNs, spleen, and ileum, obtained from donors ranging in age from 5 days to 67 years of age. Our data show that the main reservoir of polyclonal naive cells is found in the LNs, and the resting memory subsets capable of self‐renewal are also prominent there. In contrast, nondividing but functionally active memory subsets dominate the spleen, and especially the ileum. In general, the replacement of naive cells with memory subsets continues throughout our period of observation, with no apparent plateau. In conclusion, the analysis of lymphoid and nonlymphoid tissues reveals a dynamic pattern of changes distinct to each tissue, and with substantial differences between CD4+ and CD8+ compartments.
机译:摘要长期检测T细胞记忆是依赖维护的记忆T细胞淋巴组织,在表面接口为病原体提供入口路线。当前的信息对人类T细胞记忆基于循环分析T细胞。我们学习了地理分布和年龄相关的变化的内存检测T细胞在样本子集血液、肠系膜LNs脾脏和回肠,从捐赠者获得年龄在5天到67岁。储层多克隆的细胞中发现的LNs,内存子集能够休息的自我更新也应承担的突出。相反,:但功能活跃内存子集主导脾脏和尤其是回肠。天真的细胞记忆子集仍在继续在我们的观察,没有明显的高原。淋巴和nonlymphoid组织揭示了一个动态变化的模式不同组织和实质性的差异CD4 +和CD8 +隔间。

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