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Eosinophil microRNAs Play a Regulatory Role in Allergic Diseases Included in the Atopic March

机译:嗜酸性粒细胞microRNA在Atopic 3月份的过敏性疾病中起着监管作用

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摘要

(1) Background: The atopic march is defined by the increased prevalence of allergic diseases after atopic dermatitis onset. In fact, atopic dermatitis is believed to play an important role in allergen sensitization via the damaged skin barrier, leading to allergic diseases such as allergic asthma and allergic rhinitis. The eosinophil, a pro-inflammatory cell that contributes to epithelial damage, is one of the various cells recruited in the inflammatory reactions characterizing these diseases. Few studies were conducted on the transcriptome of this cell type and even less on their specific microRNA (miRNA) profile, which could modulate pathogenesis of allergic diseases and clinical manifestations post-transcriptionally. Actually, their implication in allergic diseases is not fully understood, but they are believed to play a role in inflammation-related patterns and epithelial cell proliferation. (2) Methods: Next-generation sequencing was performed on RNA samples from eosinophils of individuals with atopic dermatitis, atopy, allergic rhinitis and asthma to obtain differential counts of primary miRNA (pri-miRNA); these were also analyzed for asthma-related phenotypes such as forced expiratory volume in one second (FEV1), immunoglobulin E (IgE) and provocative concentration of methacholine inducing a 20% fall in forced expiratory volume in 1 s (PC20) levels, as well as FEV1 to forced vital capacity (FEV1/FVC) ratio. (3) Results: Eighteen miRNAs from eosinophils were identified to be significantly different between affected individuals and unaffected ones. Based on counts from these miRNAs, individuals were then clustered into groups using Ward’s method on Euclidian distances. Groups were found to be explained by asthma diagnosis, familial history of respiratory diseases and allergic rhinitis as well as neutrophil counts. (4) Conclusions: The 18 differential miRNA counts for the studying phenotypes allow a better understanding of the epigenetic mechanisms underlying the development of the allergic diseases included in the atopic march.
机译:(1)背景:应具体3月由特应性皮炎发病后过敏性疾病的流行增加。事实上,据信以特应性皮炎通过受损的皮肤屏障在过敏原致敏中发挥着重要作用,导致过敏性疾病如过敏性哮喘和过敏性鼻炎。嗜酸性粒细胞,一种有助于上皮损伤的促炎细胞,是在表征这些疾病的炎症反应中募集的各种细胞之一。在这种细胞类型的转录组上进行了很少的研究,甚至更少地对其特定的microRNA(miRNA)型材,这可以调节转录后过敏性疾病和临床表现的发病机制。实际上,它们对过敏性疾病的含义尚不完全理解,但它们被认为在炎症相关的模式和上皮细胞增殖中发挥作用。 (2)方法:下一代测序对来自特应性皮炎,特拉内,过敏性鼻炎和哮喘的个体嗜酸性血粒细胞的RNA样品进行,以获得原发性miRNA(PRI-miRNA)的差异计数;对于哮喘相关表型,例如强制呼气量在一秒(FEV1)中,免疫球蛋白E(IgE)和甲素的挑衅性浓度,甲素诱导呼气量为1 s(PC20)水平的强制呼气量,致血管蛋白e(IgE)和挑衅性浓度作为FEV1以强制生命能力(FEV1 / FVC)比率。 (3)结果:鉴定来自嗜酸性粒细胞的18只MIRNA在受影响的个体和未受影响的嗜酸性的情况下显着差异。基于这些miRNA的计数,然后使用Ward的欧几里德距离的方法将个体聚集成群体。发现血液诊断,呼吸系统疾病和过敏性鼻炎以及中性粒细胞计数的哮喘诊断。 (4)结论:研究表型的18个差异miRNA计数允许更好地了解题为外部3月份的过敏性疾病发展的表观遗传机制。

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