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首页> 外文期刊>Clinical and experimental allergy : >Uncontrolled asthmatics have increased FceRI + + and TGF‐β–positive MC TC TC mast cells and collagen VI in the alveolar parenchyma
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Uncontrolled asthmatics have increased FceRI + + and TGF‐β–positive MC TC TC mast cells and collagen VI in the alveolar parenchyma

机译:不受控制的哮喘患者在肺泡实质中增加Fceri + +和TGF-β阳性MC TC TC肥大肥料和胶原蛋白VI

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摘要

Summary Background Asthma has been associated with increased collagen deposition in both conducting airways and alveolar parenchyma. Mast cells (MCs) are key effector cells in asthma and have the ability to affect collagen synthesis. However, the link between clinical control and changes in bronchial and alveolar MC phenotypes and specific collagens in controlled and uncontrolled asthma remains unknown. Objective To investigate MC phenotypes in correlation with deposition of specific collagen subtypes in patients with controlled and uncontrolled asthma as well as to healthy controls. Methods The tissue expression of IgE + , FcεRI + and TGF‐β + MCs, as well as immunoreactivity of collagen I, III and VI, was assessed using immunohistochemistry on bronchial and transbronchial biopsies from controlled asthmatics (n?=?9), uncontrolled asthmatics (n?=?16) and healthy controls (n?=?8). Results In the alveolar parenchyma, the total number of MCs, as well as the number of FcεRI + MCs and pro‐fibrotic TGF‐β + MC TC, was significantly increased in uncontrolled asthma compared to both controlled asthma and healthy controls. The proportion of TGF‐β + MC TC correlated positively to an increased immunoreactivity of alveolar collagen VI but not collagen I and III. Collagen VI was increased in the alveolar parenchyma of uncontrolled asthmatics compared to controlled asthmatics. Controlled asthmatics had an increased deposition of alveolar collagen I. In bronchi, the immunoreactivity of collagen I was increased in both controlled and uncontrolled asthmatics while collagen III was increased only in controlled asthmatics. Conclusions Patients with uncontrolled atopic asthma have an altered pro‐fibrotic MC TC phenotype in the alveolar parenchyma that is associated with alveolar collagen VI. The present data thus support distal lung mast cell and matrix changes as histopathological features of asthma that may be of particular clinical relevance in patients who have remaining symptoms despite conventional inhaler therapy.
机译:发明内容背景哮喘与导电通气道和肺泡实质的胶原沉积增加有关。肥大细胞(MCS)是哮喘的关键效应细胞,具有影响胶原合成的能力。然而,临床控制与支气管和肺泡MC表型的变化与受控和不受控制的哮喘的特异性胶原蛋白之间的联系仍然未知。目的探讨CM表型与受控哮喘患者的特定胶原亚型的相关性及健康对照。方法使用免疫组织化学对来自受控哮喘的支气管和跨界活组织检查的免疫组化评估IgE +,FcεRI+和TGF-β+ MCS的组织表达,以及胶原I,III和VI的免疫反应性(N?=Δ9),不受控制哮喘(n?=?16)和健康对照(n?=?8)。结果肺泡实质,与受控哮喘和健康对照相比,在不受控制的哮喘相比,MCS总数以及FcεRI+ MCS和促纤维化TGF-β+ MC TC的数量显着增加。 TGF-β+ MC TC的比例呈正相关,与肺泡胶原VI的增加的免疫反应性,但不是胶原蛋白I和III。与受控哮喘学相比,在不受控制的哮喘患者的肺泡实质中增加了胶原蛋白VI。受控的哮喘患者沉积肺泡胶原I.在支气管中,在受控和不受控制的哮喘中,胶原蛋白I的免疫反应性,而胶原III仅在受控哮喘中增加。结论患有不受控制的特征性哮喘的患者在肺泡实质中具有改变的Pro-Fibriotic MC Tc表型,与肺泡胶原VI相关。因此,目前的数据支持远端肺肥蜂窝细胞和基质变化作为哮喘的组织病理学特征,尽管常规吸入器治疗,但仍可能具有剩余症状的患者的临床相关性。

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