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Two-Track Medical Treatment Strategy According to the Clinical Scoring System for Chronic Rhinosinusitis

机译:根据慢性鼻-鼻窦炎临床评分系统的两种治疗策略

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Purpose The previously reported Japanese clinical scoring study (JESREC) suggests that chronic rhinosinusitis (CRS) can be divided into 4 subtypes according to the degree of eosinophilic CRS (ECRS) and offers the information regarding the prognosis of CRS to clinicians. However, this scoring system has not yet been validated by an immunological study and needs to provide treatment guidelines based on underlying immunologic profiles. We investigated the immunologic profile of each CRS subgroup according to the JESREC classification and suggest its clinical application. Methods A total of 140 CRS patients and 20 control subjects were enrolled. All patients were classified into 4 groups according to the JESREC (non-, mild, moderate and severe ECRS). Nasal tissues were analyzed for mRNA expression of major cytokines (IL-5, IL-10, IL-13, IL-17A, IL-22, IL-23p19, IFN-γ, periostin, thymic stromal lymphopoietin [TSLP] and ST2), major chemokines (CCL11, CCL24, CXCL1 and CXCL2), transcription factors (T-bet, GATA3, RORC and FOXP3) and COL1A1 for type I collagen. Protein levels of 3 major cytokines (IL-5, IL-17A and IFN-γ) were also measured by multiplex immunoassay. Principal component analysis (PCA) was conducted to investigate the overall profile of multiple mediators. Results The moderate/severe ECRS showed up-regulation of type 2-related mediators (IL-5, IL-13, periostin, TSLP and ST-2), whereas INF-γ (type 1 cytokine) and CXCL1 (neutrophil chemokine) expressions were increased in non-/mild ECRS compared with moderate/severe ECRS. The JESREC classification reflected an immunological endotype. In PCA data, PCA1 indicates a relative type 2 profile, whereas PCA2 represents a type 1/type 17-related profile. In this analysis, mild ECRS was indistinguishable from non-ECRS, whereas moderate to severe ECRS showed a distinct distribution compared with non-ECRS. The JESREC classification could be divided into 2 categories, non-/mild vs. moderate/severe ECRS based on underlying immunological analyses. Conclusions The CRS clinical scoring system from the JESREC study reflects an inflammatory endotype. However, the immunologic profile of mild ECRS was similar to that of non-ECRS. Therefore, we propose type 2-targeted medical treatment for moderate to severe ECRS and type 1/type 17-targeted for non-ECRS and mild ECRS as the first treatment option.
机译:目的先前报道的日本临床评分研究(JESREC)表明,慢性鼻鼻窦炎(CRS)可以根据嗜酸性CRS(ECRS)的程度分为4种亚型,并向临床医生提供有关CRS预后的信息。但是,该评分系统尚未通过免疫学研究验证,需要根据潜在的免疫学概况提供治疗指导。我们根据JESREC分类调查了每个CRS亚组的免疫学特征,并提出了其临床应用。方法纳入140例CRS患者和20例对照受试者。根据JESREC将所有患者分为4组(非,轻度,中度和重度ECRS)。分析鼻腔组织中主要细胞因子(IL-5,IL-10,IL-13,IL-17A,IL-22,IL-23p19,IFN-γ,骨膜素,胸腺基质淋巴细胞生成素[TSLP]和ST2)的mRNA表达,I型胶原的主要趋化因子(CCL11,CCL24,CXCL1和CXCL2),转录因子(T-bet,GATA3,RORC和FOXP3)和COL1A1。还通过多重免疫测定法测量了三种主要细胞因子(IL-5,IL-17A和IFN-γ)的蛋白质水平。进行了主成分分析(PCA),以调查多种介体的整体情况。结果中度/重度ECRS显示2型相关介体(IL-5,IL-13,骨膜素,TSLP和ST-2)上调,而INF-γ(1型细胞因子)和CXCL1(中性粒细胞趋化因子)表达上调。非/轻度ECRS与中度/重度ECRS相比有所增加。 JESREC分类反映了免疫学内型。在PCA数据中,PCA1表示相对类型2的配置文件,而PCA2表示类型1 /类型17相关的配置文件。在此分析中,轻度ECRS与非ECRS没有区别,而中度至重度ECRS与非ECRS相比显示出明显的分布。根据基本的免疫学分析,JESREC的分类可分为两类,非/轻度与中度/重度ECRS。结论JESREC研究的CRS临床评分系统反映出炎性内型。但是,轻度ECRS的免疫学特征与非ECRS相似。因此,我们建议针对中度至重度ECRS的2型靶向治疗以及针对非ECRS和轻度ECRS的1型/ 17型靶向治疗为首选治疗方案。

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