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生物膜刺激的上皮细胞调节共培养免疫细胞中的炎症反应。

Biofilm-stimulated epithelium modulates the inflammatory responses in co-cultured immune cells.

机构信息

Institute of Biomedical and Environmental Health Research, School of Science and Sport, University of the West of Scotland, Paisley, PA1 2BE, UK.

Oral Sciences Research Group, Glasgow Dental School, School of Medicine, College of Medical, Veterinary and Life Sciences, University of Glasgow, Glasgow, G12 8TA, UK.

出版信息

Sci Rep. 2019 Oct 31;9(1):15779. doi: 10.1038/s41598-019-52115-7.

Abstract

The gingival epithelium is a physical and immunological barrier to the microbiota of the oral cavity, which interact through soluble mediators with the immune cells that patrol the tissue at the gingival epithelium. We sought to develop a three-dimensional gingivae-biofilm interface model using a commercially available gingival epithelium to study the tissue inflammatory response to oral biofilms associated with "health", "gingivitis" and "periodontitis". These biofilms were developed by sequential addition of microorganisms to mimic the formation of supra- and sub-gingival plaque in vivo. Secondly, to mimic the interactions between gingival epithelium and immune cells in vivo, we integrated peripheral blood mononuclear cells and CD14 monocytes into our three-dimensional model and were able to assess the inflammatory response in the immune cells cultured with and without gingival epithelium. We describe a differential inflammatory response in immune cells cultured with epithelial tissue, and more so following incubation with epithelium stimulated by "gingivitis-associated" biofilm. These results suggest that gingival epithelium-derived soluble mediators may control the inflammatory status of immune cells in vitro, and therefore targeting of the epithelial response may offer novel therapies. This multi-cellular interface model, both of microbial and host origin, offers a robust in vitro platform to investigate host-pathogens at the epithelial surface.

摘要

牙龈上皮是口腔微生物群的物理和免疫屏障,通过可溶性介质与在牙龈上皮处巡逻组织的免疫细胞相互作用。我们试图使用市售的牙龈上皮开发一种三维牙龈-生物膜界面模型,以研究组织对与“健康”、“牙龈炎”和“牙周炎”相关的口腔生物膜的炎症反应。这些生物膜通过顺序添加微生物来模拟体内龈上和龈下斑块的形成。其次,为了模拟体内牙龈上皮和免疫细胞之间的相互作用,我们将外周血单核细胞和 CD14 单核细胞整合到我们的三维模型中,并能够评估在有和没有牙龈上皮的情况下培养的免疫细胞的炎症反应。我们描述了在培养有上皮组织的免疫细胞中存在差异的炎症反应,并且在用“与牙龈炎相关”生物膜刺激的上皮孵育后,这种反应更为明显。这些结果表明,牙龈上皮衍生的可溶性介质可能在体外控制免疫细胞的炎症状态,因此靶向上皮反应可能提供新的治疗方法。这种源自微生物和宿主的多细胞界面模型为研究上皮表面的宿主病原体提供了一个强大的体外平台。

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