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首页> 外文期刊>Allergology international: official journal of the Japanese Society of Allergology >Recent advances in understanding the roles of blood platelets in the pathogenesis of allergic inflammation and bronchial asthma
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Recent advances in understanding the roles of blood platelets in the pathogenesis of allergic inflammation and bronchial asthma

机译:理解血小板在过敏性炎症和支气管哮喘发病机理中的作用的最新进展

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Platelets play an essential role in hemostasis to minimize blood loss due to traumatic injury. In addition, they contain various immune-associated molecules and contribute to immunological barrier formation at sites of vascular injury, thereby protecting against invading pathogens. Platelets are also crucially involved in development of allergic diseases, including bronchial asthma. Platelets in asthmatics are more activated than those in healthy individuals. By using a murine asthma model, platelets were shown to be actively involved in progression of the disease, including in airway eosinophilia and airway remodeling. In the asthmatic airway, pathological microvascular angiogenesis, a component of airway remodeling, is commonly observed, and the degree of abnormality is significantly associated with disease severity. Therefore, in order to repair the newly formed and structurally fragile blood vessels under inflammatory conditions, platelets may be continuously activated in asthmatics. Importantly, platelets constitutively express IL-33 protein, an alarmin cytokine that is essential for development of bronchial asthma. Meanwhile, the concept of development of allergic diseases has recently changed dramatically, and allergy researchers now share a belief in the centrality of epithelial barrier functions. In particular, IL-33 released from epithelial barrier tissue at sites of eczema can activate the antigen-non-specific innate immune system as an alarmin that is believed to be necessary for subsequent antigen-specific acquired immunological responses. From this perspective, we propose in this review a possible mechanism for how activated platelets act as an alarmin in development of bronchial asthma.
机译:血小板在止血中起着至关重要的作用,以最大程度地减少由于创伤造成的失血。此外,它们包含各种免疫相关分子,并有助于在血管损伤部位形成免疫屏障,从而防止入侵病原体。血小板还严重参与过敏性疾病的发展,包括支气管哮喘。哮喘患者中的血小板比健康个体中的血小板活化更多。通过使用鼠类哮喘模型,显示血小板积极参与疾病的进展,包括气道嗜酸性粒细胞增多和气道重塑。在哮喘气道中,通常观察到病理性微血管血管生成(气道重塑的一个组成部分),异常程度与疾病严重程度显着相关。因此,为了在炎症条件下修复新形成的结构脆弱的血管,可以在哮喘患者中连续激活血小板。重要的是,血小板组成性表达IL-33蛋白,这是警报蛋白,对支气管哮喘的发展至关重要。同时,过敏性疾病发展的概念最近发生了巨大变化,过敏研究人员现在对上皮屏障功能的中心性有共同的信念。特别地,在湿疹部位从上皮屏障组织释放的IL-33可以激活非抗原特异性先天免疫系统作为警报蛋白,据认为对于随后的抗原特异性获得性免疫应答是必需的。从这个角度出发,我们在本综述中提出了活化的血小板如何在支气管哮喘发展中充当警报蛋白的可能机制。

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