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首页> 外文期刊>Journal of otolaryngology - head & neck surgery = >Simple hypertrophic tonsils have more active innate immune and inflammatory responses than hypertrophic tonsils with recurrent inflammation in children
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Simple hypertrophic tonsils have more active innate immune and inflammatory responses than hypertrophic tonsils with recurrent inflammation in children

机译:比儿童复发炎症的肥厚扁桃体有更具活跃的肥大扁桃体,肥厚性免疫和炎症反应

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摘要

Tonsil hypertrophy has negative impact on children’s health, but its pathogenesis remains obscure despite the fact that numerous bacteriological studies have been carried out. Understanding the innate immune and inflammatory states of hypertrophic tonsils with different clinical manifestations is of great significance for defining the pathogenesis of tonsil hypertrophy and establishing treatment strategies. The present study was undertaken to examine the characteristics of innate immunity and inflammation in children with hypertrophic palatine tonsils and different clinical manifestations. Tonsil tissues were surgically removed from the patients and classified based on the patients’ clinical manifestations. The patients were divided into three groups: 1) Control group; 2) Tonsil Hypertrophy (TH) group; and 3) Tonsil Hypertrophy combined with Recurrent Infection (TH?+?RI) group. The immune and inflammatory statuses of these tissues were characterized using qRT-PCR and ELISA methods. Viral protein 1 (VP1) was highly expressed in TH group, but not in TH?+?RI group. In TH group, elevated expression was observed in the innate immune mediators, including retinoic acid-inducible gene I (RIG-I), interferon alpha (IFN-α), mitochondrial antiviral-signaling protein (MAVS), NLR family pyrin domain containing 3 (NLRP3), toll-like receptor (TLR) 4 and TLR7. Consistent with the innate immune profile, the expression of inflammatory markers (IL-1β, NF-κB and IL-7) was also significantly elevated in TH group. Meanwhile, the COX-2/PGE2/EP4 signaling pathway was found to be involved in the inflammatory response and the formation of fibroblasts. Innate immune and inflammatory responses are more active in simple hypertrophic tonsils, rather than hypertrophic tonsils with recurrent inflammation. A local relative immune deficiency in the hypertrophic tonsils may be a causative factor for recurrent tonsillitis in TH?+?RI. These differences, together with the patient’s clinical manifestations, suggest that tonsillar hypertrophy might be regulated by diverse immune and/or inflammatory mechanism through which novel therapeutic strategies might be created.
机译:扁桃体肥大对儿童健康产生负面影响,但其发病机制仍然是模糊的,尽管已经进行了许多细菌学研究。了解具有不同临床表现的肥厚扁桃体的先天免疫和炎症状态对于定义扁桃体肥大和建立治疗策略的发病机制具有重要意义。本研究旨在探讨肥大腭扁桃体和不同临床表现儿童先天免疫和炎症的特征。根据患者的临床表现,手术从患者中移除扁桃体组织并分类。患者分为三组:1)对照组; 2)扁桃体肥大(TH)组; 3)扁桃体肥大结合反复感染(Th?+ΔRI)组。使用QRT-PCR和ELISA方法表征这些组织的免疫和炎症状态。病毒蛋白1(VP1)在Th组中高度表达,但不是在α+αri组中。在Th组中,在先天免疫介质中观察到升高的表达,包括视黄酸 - 诱导基因I(RIG-I),干扰素α(IFN-α),线粒体抗病算子(MAVS),NLR家族吡林结构域,含有3 (NLRP3),易于接受受体(TLR)4和TLR7。与先天免疫分布一致,炎症标记物(IL-1β,NF-κB和IL-7)的表达也在群体中显着升高。同时,发现COX-2 / PGE2 / EP4信号通路参与炎症反应和成纤维细胞的形成。先天免疫和炎症反应在简单的肥大扁桃体中更活跃,而不是具有复发性炎症的肥厚扁桃体。肥大扁桃体中的局部相对免疫缺乏可能是炎症扁桃体炎的致病因素+?ri。这些差异与患者的临床表现相同表明,扁桃体肥大可能受到不同的免疫和/或炎症机制,通过该机制可能会产生新的治疗策略。

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