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树突状细胞和巨噬细胞形成一个针对外来颗粒抗原的跨上皮网络。

Dendritic cells and macrophages form a transepithelial network against foreign particulate antigens.

作者信息

Blank Fabian, Rothen-Rutishauser Barbara, Gehr Peter

机构信息

Institute of Anatomy, Division of Histology, University of Bern, Baltzerstrasse 2, CH-3000 Bern 9, Switzerland.

出版信息

Am J Respir Cell Mol Biol. 2007 Jun;36(6):669-77. doi: 10.1165/rcmb.2006-0234OC. Epub 2007 Feb 1.

Abstract

Fine particles (0.1-2.5 microm in diameter) may cause increased pulmonary morbidity and mortality. We demonstrate with a cell culture model of the human epithelial airway wall that dendritic cells extend processes between epithelial cells through the tight junctions to collect particles in the "luminal space" and to transport them through cytoplasmic processes between epithelial cells across the epithelium or to transmigrate through the epithelium to take up particles on the epithelial surface. Furthermore, dendritic cells interacted with particle-loaded macrophages on top of the epithelium and with other dendritic cells within or beneath the epithelium to take over particles. By comparing the cellular interplay of dendritic cells and macrophages across epithelial monolayers of different transepithelial electrical resistance, we found that more dendritic cells were involved in particle uptake in A549 cultures showing a low transepithelial electrical resistance compared with dendritic cells in16HBE14o cultures showing a high transepithelial electrical resistance 10 min (23.9% versus 9.5%) and 4 h (42.1% versus 14.6%) after particle exposition. In contrast, the macrophages in A549 co-cultures showed a significantly lower involvement in particle uptake compared with 16HBE14o co-cultures 10 min (12.8% versus 42.8%) and 4 h (57.4% versus 82.7%) after particle exposition. Hence we postulate that the epithelial integrity influences the particle uptake by dendritic cells, and that these two cell types collaborate as sentinels against foreign particulate antigen by building a transepithelial interacting cellular network.

摘要

细颗粒物(直径0.1 - 2.5微米)可能会导致肺部发病率和死亡率上升。我们利用人呼吸道上皮细胞的细胞培养模型证明,树突状细胞通过紧密连接在上皮细胞之间伸出突起,在“管腔空间”收集颗粒,并通过上皮细胞之间的细胞质突起将颗粒转运穿过上皮,或通过上皮迁移以摄取上皮表面的颗粒。此外,树突状细胞与上皮表面的载有颗粒的巨噬细胞以及上皮内或上皮下的其他树突状细胞相互作用以摄取颗粒。通过比较不同跨上皮电阻的上皮单层中树突状细胞和巨噬细胞的细胞相互作用,我们发现,与跨上皮电阻高的16HBE14o培养物中的树突状细胞相比,跨上皮电阻低的A549培养物中有更多树突状细胞参与颗粒摄取,在颗粒暴露后10分钟(23.9%对9.5%)和4小时(42.1%对14.6%)。相反,与颗粒暴露后10分钟(12.8%对42.8%)和4小时(57.4%对82.7%)的16HBE14o共培养物相比,A549共培养物中的巨噬细胞参与颗粒摄取的比例明显更低。因此,我们推测上皮完整性会影响树突状细胞对颗粒的摄取,并且这两种细胞类型通过构建跨上皮相互作用的细胞网络,作为抵御外来颗粒抗原的哨兵协同作用。

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