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用嗜肺军团菌对小鼠中耳上皮细胞重塑进行超稳定同位素标记氨基酸定量蛋白质组分析

SuperSILAC Quantitative Proteome Profiling of Murine Middle Ear Epithelial Cell Remodeling with NTHi.

作者信息

Val Stéphanie, Burgett Katelyn, Brown Kristy J, Preciado Diego

机构信息

Sheikh Zayed Center for Pediatric Surgical Innovation, Children's National Health System, Washington, DC, United States of America.

Center for Genetic Medicine Research, Children's National Health System, Washington, DC, United States of America.

出版信息

PLoS One. 2016 Feb 9;11(2):e0148612. doi: 10.1371/journal.pone.0148612. eCollection 2016.

Abstract

BACKGROUND

Chronic Otitis Media with effusion (COME) develops after sustained inflammation and is characterized by secretory middle ear epithelial metaplasia and effusion, most frequently mucoid. Non-typeable Haemophilus influenzae (NTHi), the most common acute Otitis Media (OM) pathogen, is postulated to promote middle ear epithelial remodeling in the progression of OM from acute to chronic. The goals of this study were to examine histopathological and quantitative proteomic epithelial effects of NTHi challenge in a murine middle ear epithelial cell line.

METHODS

NTHi lysates were generated and used to stimulate murine epithelial cells (mMEEC) cultured at air-liquid interface over 48 hours- 1 week. Conditional quantitative Stable Isotope Labeling with Amino Acids in Cell Culture (SILAC) of cell lysates was performed to interrogate the global protein production in the cells, using the SuperSILAC technique. Histology of the epithelium over time was done to measure bacterial dependent remodeling.

RESULTS

Mass spectrometry analysis identified 2,565 proteins across samples, of which 74 exhibited differential enrichment or depletion in cell lysates (+/-2.0 fold-change; p value<0.05). The key molecular functions regulated by NTHi lysates exposure were related to cell proliferation, death, migration, adhesion and inflammation. Finally, chronic exposure induced significant epithelial thickening of cells grown at air liquid interface.

CONCLUSIONS

NTHi lysates drive pathways responsible of cell remodeling in murine middle ear epithelium which likely contributes to observed epithelial hyperplasia in vitro. Further elucidation of these mediators will be critical in understanding the progression of OM from acute to chronic at the molecular level.

摘要

背景

分泌性中耳炎(COME)在持续性炎症后发生,其特征为中耳上皮化生和积液,最常见的是黏液样积液。不可分型流感嗜血杆菌(NTHi)是最常见的急性中耳炎(OM)病原体,据推测在OM从急性向慢性进展过程中促进中耳上皮重塑。本研究的目的是在小鼠中耳上皮细胞系中研究NTHi刺激对组织病理学和定量蛋白质组学上皮的影响。

方法

制备NTHi裂解物,并用于刺激在气液界面培养48小时至1周的小鼠上皮细胞(mMEEC)。使用SuperSILAC技术对细胞裂解物进行细胞培养中氨基酸的条件性定量稳定同位素标记(SILAC),以探究细胞中的整体蛋白质产生情况。对上皮进行随时间的组织学检查,以测量细菌依赖性重塑。

结果

质谱分析在各样本中鉴定出2565种蛋白质,其中74种在细胞裂解物中表现出差异富集或消耗(变化倍数为±2.0;p值<0.05)。NTHi裂解物暴露所调节的关键分子功能与细胞增殖、死亡、迁移、黏附和炎症有关。最后,慢性暴露导致在气液界面生长的细胞出现明显的上皮增厚。

结论

NTHi裂解物驱动小鼠中耳上皮细胞重塑的相关通路,这可能导致体外观察到的上皮增生。进一步阐明这些介质对于在分子水平理解OM从急性向慢性的进展至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ff29/4747582/b69a1cf70191/pone.0148612.g001.jpg

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