Pérez-Pazos Jacqueline, García-Sánchez Asunción, Estravís Miguel, Moreno-Jimenez Emma, Morgado Natalia, Gómez-García Manuel, Ramos-González Jacinto, Gil-Melcón María, Martín-García Cristina, Muñoz-Bellido Francisco, Sanz Catalina, Isidoro-García María, Dávila Ignacio
Instituto de Investigación Biomédica de Salamanca, Salamanca, Spain.
Hospital Universitario de Salamanca, Pharmacogenetics and Precision Medicine Unit, Clinical Biochemistry Department, Salamanca, Spain.
ERJ Open Res. 2024 Aug 5;10(4). doi: 10.1183/23120541.00909-2023. eCollection 2024 Jul.
Type 2 (T2) asthma is often associated with chronic rhinosinusitis with nasal polyposis (CRSwNP). Additionally, nonsteroidal anti-inflammatory drug (NSAID) intolerance leads to NSAID-exacerbated respiratory disease (N-ERD). Previous transcriptomic data in non-CRSwNP T2 asthma patients showed differentially expressed genes. We focused on , , , and to investigate their role in T2 asthma.
The study included 100 healthy controls and 103 T2 asthma patients, divided into patients with asthma (n=54), patients with asthma and CRSwNP (n=29) and patients with N-ERD (n=20). Quantitative PCR analysis was performed on blood-derived RNA samples first to validate the five differentially expressed genes. The data were further analysed to find potential associations and biomarkers.
Patients, regardless of stratification, exhibited significantly higher gene expression than healthy controls. The patterns of association revealed that was exclusively present in the non-comorbidity group, and in the comorbidity groups, and in all patient groups. , and expression showed potential as biomarkers to confirm the diagnosis of T2 asthma using peripheral blood eosinophils as the initial criterion. Peripheral blood eosinophils combined with gene expression, especially , may improve the diagnosis. and expression play a specific role in discriminating N-ERD.
We validated the transcriptomic data of five differentially expressed genes in T2 asthma. Different patterns of association were identified in patient stratification, suggesting that different molecular mechanisms underlie the spectrum of T2 asthma. Potential biomarkers were also found and used to design an algorithm with practical diagnostic utility for T2 asthma, including risk stratification for N-ERD.
2型(T2)哮喘常与伴有鼻息肉的慢性鼻-鼻窦炎(CRSwNP)相关。此外,非甾体抗炎药(NSAID)不耐受会导致NSAID加重的呼吸道疾病(N-ERD)。既往非CRSwNP T2哮喘患者的转录组数据显示存在差异表达基因。我们聚焦于[具体基因名称1]、[具体基因名称2]、[具体基因名称3]、[具体基因名称4]和[具体基因名称5],以研究它们在T2哮喘中的作用。
该研究纳入100名健康对照者和103名T2哮喘患者,分为哮喘患者(n = 54)、哮喘合并CRSwNP患者(n = 29)和N-ERD患者(n = 20)。首先对血液来源的RNA样本进行定量PCR分析,以验证这五个差异表达基因。进一步分析数据以寻找潜在关联和生物标志物。
无论分层如何,患者的基因表达均显著高于健康对照者。关联模式显示,[具体基因名称1]仅存在于无合并症组,[具体基因名称2]和[具体基因名称3]存在于合并症组,[具体基因名称4]存在于所有患者组。[具体基因名称5]、[具体基因名称4]和[具体基因名称3]的表达显示出作为生物标志物的潜力,可以外周血嗜酸性粒细胞作为初始标准来确诊T2哮喘。外周血嗜酸性粒细胞与基因表达相结合,尤其是[具体基因名称5],可能会改善诊断。[具体基因名称2]和[具体基因名称1]的表达在鉴别N-ERD中起特定作用。
我们验证了T2哮喘中五个差异表达基因的转录组数据。在患者分层中发现了不同的关联模式,这表明T2哮喘谱背后存在不同的分子机制。还发现了潜在的生物标志物,并用于设计一种对T2哮喘具有实际诊断效用算法,包括N-ERD的风险分层。
