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Ezrin a Membrane Cytoskeleton Cross-Linker Protein as a Marker of Epithelial Damage in Asthma

机译:Ezrin是一种膜细胞骨架交联蛋白是哮喘上皮损伤的标志物

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摘要

>Rationale: Bronchial epithelial cell damage occurs in patients with bronchial asthma. Ezrin, a membrane-cytoskeleton protein, maintains cellular morphology and intercellular adhesion and protects the barrier function of epithelial cells.>Objectives: To study the role of ezrin in bronchial epithelial cells injury and correlate its expression with asthma severity.>Methods: Levels of ezrin were measured in exhaled breath condensate (EBC) and serum in patients with asthma and BAL fluid (BALF) from a mouse model of asthma by ELISA. The regulation of IL-13 on ezrin protein levels was studied in primary bronchial epithelial cells. Ezrin knockdown using shRNA was studied in human bronchial epithelial 16HBE cells.>Measurements and Main Results: Ezrin levels were decreased in asthmatic EBC (92.7 ± 34.99 vs. 150.5 ± 10.22 pg/ml, P < 0.0001) and serum (700.7 ± 55.59 vs. 279.2 ± 25.83 pg/ml, P < 0.0001) compared with normal subjects. Levels were much lower in uncontrolled (P < 0.001) and partly controlled patients (P < 0.01) compared with well-controlled subjects. EBC and serum ezrin levels correlated with lung function in patients with asthma and serum ezrin levels were negatively correlated with serum IL-13 and periostin. IL-13–induced downregulation of ezrin expression in primary bronchial epithelial cells was significantly attenuated by the Janus tyrosine kinase 2 inhibitor, TG101348. Ezrin knockdown changed 16HBE cell morphology, enlarged intercellular spaces, and increased their permeability. Ezrin expression was decreased in the lung tissue and BALF of “asthmatic” mice and negatively correlated with BALF IL-13 level.>Conclusions: Ezrin downregulation is associated with IL-13–induced epithelial damage and might be a potential biomarker of asthma control.
机译:>原理:支气管哮喘患者发生支气管上皮细胞损伤。膜细胞骨架蛋白Ezrin维持细胞形态和细胞间粘附并保护上皮细胞的屏障功能。>目的:研究ezrin在支气管上皮细胞损伤中的作用并将其表达与哮喘严重程度相关。>方法:用ELISA法测定哮喘小鼠的哮喘和BAL液(BALF)患者的呼出气冷凝物(EBC)和血清中的ezrin水平。在原发性支气管上皮细胞中研究了IL-13对ezrin蛋白水平的调节。在人支气管上皮16HBE细胞中研究了使用shRNA进行的Ezrin敲除。>测量和主要结果:哮喘EBC中Ezrin水平降低(分别为92.7±34.99和150.5±10.22 pg / ml,P <0.0001)和血清(700.7±55.59 vs. 279.2±25.83 pg / ml,P <0.0001)。与完全控制的受试者相比,未控制(P 0.001)和部分控制的患者(P <0.01)的水平要低得多。哮喘患者的EBC和血清ezrin水平与肺功能相关,血清ezrin水平与血清​​IL-13和骨膜素呈负相关。 Janus酪氨酸激酶2抑制剂TG101348显着减弱了IL-13诱导的支气管上皮细胞中ezrin表达的下调。 Ezrin组合式改变了16HBE细胞形态,扩大了细胞间隙,并增加了其通透性。 Ezrin在“哮喘”小鼠的肺组织和BALF中表达降低,并且与BALF IL-13水平呈负相关。>结论: Ezrin下调与IL-13诱导的上皮损伤有关,可能是由于控制哮喘的潜在生物标志物。

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