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T 细胞-树突状细胞相互作用动力学在诱导呼吸耐受和免疫中的作用。

T cell-dendritic cell interaction dynamics during the induction of respiratory tolerance and immunity.

机构信息

Institute of Immunology, Hannover Medical School, Hannover, Germany.

出版信息

J Immunol. 2010 Feb 1;184(3):1317-27. doi: 10.4049/jimmunol.0902277. Epub 2009 Dec 30.

Abstract

Dendritic cells (DCs) residing in the lung are known to acquire inhaled Ag and, after migration to the draining bronchial lymph node (brLN), to present it to naive T cells in an either tolerogenic or immunogenic context. To visualize endogenous lung-derived DCs, we applied fluorescent latex beads (LXs) intratracheally, thereby in vivo labeling the majority of phagocytic cells within the lung. Of note, LX-bearing cells subsequently arriving in the draining brLN were found to represent lung-derived migratory DCs. Imaging explanted brLN by two-photon laser-scanning microscopy, we quantitatively analyzed the migration and interaction behavior of naive CD4(+) T cells and endogenous, lung-derived DC presenting airway-delivered Ag under inflammatory or noninflammatory conditions. Ag-specific naive CD4(+) T cells engaged in stable as well as transient contacts with LX-bearing DCs in both situations and displayed similar overall motility kinetics, including a pronounced decrease in motility at 16-20 h after antigenic challenge. In contrast, the comparative analysis of T cell-DC cluster sizes as well as contact durations strongly suggests that lung-derived migratory DCs and naive CD4(+) T cells form more stable, long-lasting contacts under inflammatory conditions favoring the induction of respiratory immunity.

摘要

肺内的树突状细胞 (DCs) 已知可以摄取吸入的 Ag,然后迁移到引流的支气管淋巴结 (brLN),在耐受或免疫原性的情况下将其呈递给幼稚 T 细胞。为了可视化内源性肺来源的 DCs,我们通过气管内应用荧光乳胶珠 (LX),从而在体内标记肺内的大多数吞噬细胞。值得注意的是,随后在引流的 brLN 中发现携带 LX 的细胞代表肺来源的迁移性 DCs。通过双光子激光扫描显微镜对离体的 brLN 进行成像,我们定量分析了在炎症或非炎症条件下,幼稚 CD4(+) T 细胞和内源性、肺来源的 DC 呈递气道递呈的 Ag 的迁移和相互作用行为。在两种情况下,抗原特异性幼稚 CD4(+) T 细胞都与携带 LX 的 DC 发生稳定和短暂的接触,并表现出相似的整体迁移动力学,包括在抗原挑战后 16-20 小时迁移性显著降低。相比之下,对 T 细胞-DC 簇大小和接触持续时间的比较分析强烈表明,在炎症条件下,肺来源的迁移性 DCs 和幼稚 CD4(+) T 细胞形成更稳定、持久的接触,有利于诱导呼吸免疫。

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