Аdvanced糖基化终产物作为嗜酸性粒细胞衍生的肺部炎症性疾病的新生物标志物(文献综述)

A. Gamian, S. Zubchenko, A. Havrylyuk, I. Kril, V. Chopyak
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摘要

晚期糖基化终产物(AGEs)是在各种组织和液体的细胞糖基化过程中产生的,是由还原糖与蛋白质、脂质和核酸的氨基非酶反应形成的异质分子群。在正常情况下,它们发挥免疫调节作用。在病理条件下,AGEs激活晚期糖基化终产物(RAGE)受体并引起长期炎症。RAGE积极参与各种疾病,如类风湿关节炎、糖尿病等。然而,利用AGE在变应性疾病发病机制中的作用的可能性的科学研究相对较少。RAGE转录物和蛋白通过肺I型肺泡上皮细胞在肺中表达,提示RAGE在肺病理生理中具有重要作用。它们抑制一些内源性的自我调节功能,导致许多疾病,包括过敏。氧化应激会增加哮喘和过敏的炎症反应。持续的炎症反应伴随自由基的产生是过敏反应的重要因素,对过敏的发生和预后有不利影响。RAGEs在循环免疫细胞上表达,它们激活NF κ b,细胞内氧化应激也增加哮喘和过敏的炎症反应。膜RAGE (mRAGE)信号是促炎的,而可溶性RAGE (sRAGE)是RAGE的一种分泌形式,通常是抗炎的。研究AGEs、可溶性RAGE、RAGE配体HMGB1、S100A8/A913和IL-33作为嗜酸性粒细胞源性和中性粒细胞源性哮喘/AAD鉴别诊断的生物标志物是有用的。RAGE的平均血清水平可能是新的治疗干预措施的目标。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Аdvanced glycation end-products as novel biomarkers of eosinophil-derived lung inflammatory diseases (literature review)
Advanced glycation end-products (AGEs) are created during the process of glycation of cells from various tissues and fluids and are a heterogeneous group of molecules formed from the nonenzymatic reaction of reducing sugars with the amino group of proteins, lipids, and nucleic acid. In normal conditions, they play the immunoregulatory role. In pathologic conditions AGEs activate the receptors for advanced glycation end products (RAGE) and cause long-lasting inflammation. RAGE participates actively in various disorders such as rheumatoid arthritis, diabetes, etc. However, there is relatively small number of scientific studies on the possibility of using the role of AGE in the pathogenesis of allergic diseases. RAGE transcript and protein are expressed in the lung by pulmonary type I alveolar epithelial cells, suggesting that RAGE has an important role in lung pathophysiology. They repress some endogenous autoregulatory functions leading to many diseases, including allergy. Oxidative stress increases the inflammatory reaction in asthma and allergies. Long-lasting inflammation followed by free radicals production are important factors involved in allergic reactions, they negatively influence the incidence and prognosis of allergy. RAGEs are expressed on circulating immune cells, they activate NF kappaB and intracellular oxidative stress also increases the inflammatory reaction in asthma and allergies. The membrane RAGE (mRAGE) signaling is proinflammatory, whereas soluble RAGE (sRAGE), a secreted form of RAGE, is generally anti-inflammatory. The study of AGEs, soluble RAGE, ligands of RAGE HMGB1, and S100A8/A913 and IL-33 is useful in the context of their considering as biomarkers to the differentiation diagnostic between eosinophils-derived and neutrophil-derived asthma/AAD. The mean serum levels of RAGE may be the target of new therapeutic interventions.
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