Graves眼窝病眼眶结缔组织的高通量蛋白质组学和免疫组化研究。

Yuanping Hai, Qintao Ma, Sijie Fang, Faranak Bahramimehr, Cheng Song, Yongbo Duan, Genfeng Yu, Xiaohua Lu, Chunmei Jin, Xiao Wang, Lan Liu, Huiyu Guo, Yi Wang, Huifang Zhou, Thomas Efferth, George J Kahaly, Jie Shen
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引用次数: 0

摘要

背景:高通量蛋白质组学(HTP)有助于识别特定疾病的特征信号网络,从而在基础研究和精准医学中提供了一系列潜在的应用。免疫组织化学可以揭示局部眼眶免疫。方法:采用HPT对Graves眼病、氧化石墨烯患者(临床重度氧化石墨烯11例,轻度氧化石墨烯12例)和8例对照患者的31例眼眶结缔组织样本进行检测。我们重点研究了重度氧化石墨烯、轻度氧化石墨烯和对照组之间差异表达蛋白(DEPs)的交集。使用基因本体和京都基因与基因组百科全书对dep进行分析。使用11例重度和7例轻度氧化石墨烯眼眶组织进行免疫组化验证。免疫染色采用可靠的自动化软件进行定量分析,确保客观、独立于操作人员的评估。结果:共鉴定出4,579种蛋白:在比较轻度氧化石墨烯与对照组、重度氧化石墨烯与对照组、重度氧化石墨烯与轻度氧化石墨烯时,分别记录了847、790和208种dep(所有结论:首次将蛋白质组学和免疫组织化学相结合,检测到可能与氧化石墨烯进展有关的眶组织蛋白上调。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
High-Throughput Proteomics and Immunohistochemistry of Orbital Connective Tissue in Graves' Orbitopathy.

Background: High-throughput proteomics (HTP) helps identify characteristic signaling networks specific to certain diseases, thus offering a range of potential applications in basic research and precision medicine. Immunohistochemistry can uncover local orbital immunity.

Methods: Thirty-one orbital connective tissue samples from patients with Graves' Orbitopathy, GO (11 with clinically severe and 12 with mild GO), and from eight control subjects were examined using HPT. We focused on the intersection of differentially expressed proteins (DEPs) that differ between severe GO and both mild GO and control. Gene ontology and the Kyoto Encyclopedia of Genes and Genomes were used to analyze DEPs. Immunohistochemical verification was performed using 11 severe and 7 mild GO orbital tissues. Immunostaining was quantitatively analyzed using reliable and automated software that ensures objective, operator-independent evaluation.

Results: A total of 4,579 proteins were identified: 847, 790, and 208, DEPs were registered when comparing mild GO vs. control, severe GO vs control, and severe versus mild GO, respectively (all p<0.05). Using a cut-off threshold of fold change ≥ 2.0 during screening, five significantly up-regulated DEPs (Latent-transforming growth factor β-binding protein 2, Lysyl oxidase homolog, Ras-interacting protein 1, Integrin beta 3, Coagulation factor XII) overlapped between severe GO and both mild GO and control; while 163 up-regulated DEPs were involved in various biological processes (angiogenesis, inflammation, tissue remodeling and fibrosis). Subsequent immunohistochemical tissue validation confirmed the HTP findings.

Conclusions: For the first time, combined proteomics and immunohistochemistry detected upregulated orbital tissue proteins potentially implicated in GO progression.

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