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慢性鼻-鼻窦炎和下呼吸道疾病中的非 2 型和混合炎症。

Non-Type 2 and Mixed Inflammation in Chronic Rhinosinusitis and Lower Airway Disease.

机构信息

Division of Otolaryngology - Head and Neck Surgery, Department of Surgery, University of British Columbia, Vancouver, Canada.

出版信息

Laryngoscope. 2024 Mar;134(3):1005-1013. doi: 10.1002/lary.30992. Epub 2023 Aug 24.

Abstract

OBJECTIVE

The aim was to discuss the role of non-type 2 inflammation in patients diagnosed with chronic rhinosinusitis (CRS) and comorbid lower airway disease.

DATA SOURCES

Medline, Embase, National Institute for Health and Care Excellence, TRIP Database, ProQuest, Clinicaltrials.gov, Cochrane Central Registry of Controlled Trials, Web of Science, government and health organizations, and graduate-level theses.

REVIEW METHODS

This scoping review followed PRISMA-ScR guidelines. Search strategy was peer-reviewed by medical librarians. Studies were included if they utilized airway sampling, non-type 2 cytokines, and patients with CRS and lower airway disease.

RESULTS

Twenty-seven from 7060 articles were included. In patients with CRS and comorbid asthma, aspirin-exacerbated respiratory disease (AERD), and chronic obstructive pulmonary disease (COPD)/bronchiectasis, 60% (n = 12), 33% (n = 2), and 100% (n = 1), respectively, demonstrated mixed or non-type 2 endotypes. Comorbid CRS and asthma produced type 1 (n = 1.5), type 2 (n = 8), type 3 (n = 1), mixed type 1/2 (n = 1), and mixed type 1/2/3 (n = 8.5) endotype shifts. AERD demonstrated type 2 (n = 4), mixed type 2/3 (n = 1), and mixed type 1/2/3 (n = 1) endotype shifts. CRS with COPD or bronchiectasis demonstrated a mixed 1/2 (n = 1) endotype shift.

CONCLUSION

Type 2 disease has been extensively reviewed due to advent biologics targeting type 2 inflammation, but outcomes may be suboptimal due to the presence of non-type 2 inflammation. A proportion of patients with CRS and comorbid lower airway disease demonstrated mixed and non-type 2 endotype shifts. This emphasizes that patients with unified airway disease may have forms of inflammation beyond classical type 2 disease which could inform biologic development. Laryngoscope, 134:1005-1013, 2024.

摘要

目的

讨论非 2 型炎症在诊断为慢性鼻-鼻窦炎(CRS)和合并下气道疾病患者中的作用。

资料来源

Medline、Embase、英国国家卫生与保健优化研究所、TRIP 数据库、ProQuest、Clinicaltrials.gov、Cochrane 对照试验中心注册库、Web of Science、政府和卫生组织以及研究生论文。

检索方法

本范围综述遵循 PRISMA-ScR 指南。检索策略由医学图书馆员进行同行评审。如果研究利用气道采样、非 2 型细胞因子以及 CRS 和下气道疾病患者,则纳入研究。

结果

在患有 CRS 合并哮喘、阿司匹林加重性呼吸系统疾病(AERD)和慢性阻塞性肺疾病(COPD)/支气管扩张症的患者中,分别有 60%(n=12)、33%(n=2)和 100%(n=1)显示混合或非 2 型表型。合并 CRS 和哮喘的患者产生 1 型(n=1.5)、2 型(n=8)、3 型(n=1)、混合 1/2 型(n=1)和混合 1/2/3 型(n=8.5)表型转变。AERD 显示 2 型(n=4)、混合 2/3 型(n=1)和混合 1/2/3 型(n=1)表型转变。CRS 合并 COPD 或支气管扩张症表现出混合 1/2 型(n=1)表型转变。

结论

由于针对 2 型炎症的生物制剂问世,2 型疾病已得到广泛研究,但由于存在非 2 型炎症,结果可能并不理想。一部分患有 CRS 和合并下气道疾病的患者表现出混合和非 2 型表型转变。这强调了具有统一气道疾病的患者可能具有超出经典 2 型疾病的炎症形式,这可以为生物制剂的发展提供信息。

喉镜,134:1005-1013,2024。

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