Ying Shengjie, Zeng Peter Y F, Fung Kevin, Khan Halema, Cecchini Matthew J, Woo Elissa, Anderson Jennifer, MacInnis Patrick, Karimi Amir H, Al Jawhri MohdWessam, Pan Harrison, Le Nhi, Joris Krista, Wen Rui, Mymryk Joe S, Inculet Richard, Dumeaux Vanessa, Barrett John W, Nichols Anthony C, Lin R Jun
Department of Otolaryngology-Head and Neck Surgery, Western University, London, Ontario, Canada.
Department of Pathology and Laboratory Medicine, Western University, London, Ontario, Canada.
Laryngoscope. 2025 Sep;135(9):3273-3279. doi: 10.1002/lary.32214. Epub 2025 May 6.
Idiopathic subglottic stenosis (iSGS) is a rare disease characterized by narrowing of the upper airway and affects near-exclusively females. Patients often experience recurrent disease and require repeated surgical dilations. The pathophysiology underlying the broad spectrum of disease severity within iSGS remains unknown. In the current study, we sought to identify transcriptomic differences between iSGS patients with markedly different recurrence rates.
Prospectively collected clinical and bulk RNA sequencing data from subglottic tissues of 56 female iSGS patients with 1-4 years of follow-up were analyzed. DESeq2 was used to perform differential expression analysis, comparing samples from the highest (1.19-1.87 dilations/year) versus the lowest (0.30-0.65 dilations/year) quartile of surgical dilation rate (i.e., high vs. low recurrence groups).
In total, 220 genes were significantly differentially expressed between the high and low recurrence groups (adjusted p < 0.1 and log fold change > |1|). Pathway enrichment analyses showed that the high recurrence group had significantly increased expression of genes involved in adaptive immune responses (e.g., immunoglobulin subunit genes) and extracellular matrix organization (e.g., COMP, NID2) (adjusted p < 0.1). In contrast, the low recurrence group had significantly increased expression of genes involved in cilia structure and function (e.g., CFAP43, DNAI2) (adjusted p < 0.1), suggesting a relatively increased abundance of respiratory cilia.
Transcriptomic profiling suggests that lower recurrence rates in iSGS are associated with retention of respiratory cilia, while adaptive immune responses and increased extracellular matrix deposition are present in those with higher recurrence rates. These results hold promise for the development of prognostic markers and identification of therapeutic targets for iSGS.
特发性声门下狭窄(iSGS)是一种罕见疾病,其特征为上呼吸道狭窄,且几乎仅影响女性。患者常经历疾病复发,需要反复进行手术扩张。iSGS疾病严重程度范围广泛,其潜在的病理生理学机制仍不清楚。在本研究中,我们试图确定复发率明显不同的iSGS患者之间的转录组差异。
对前瞻性收集的56例女性iSGS患者声门下组织的临床和批量RNA测序数据进行分析,这些患者有1至4年的随访记录。使用DESeq2进行差异表达分析,比较手术扩张率最高(1.19 - 1.87次扩张/年)与最低(0.30 - 0.65次扩张/年)四分位数的样本(即高复发组与低复发组)。
高复发组和低复发组之间共有220个基因存在显著差异表达(校正p < 0.1且log倍数变化 > |1|)。通路富集分析表明,高复发组中参与适应性免疫反应(如免疫球蛋白亚基基因)和细胞外基质组织(如COMP、NID2)的基因表达显著增加(校正p < 0.1)。相比之下,低复发组中参与纤毛结构和功能(如CFAP43、DNAI2)的基因表达显著增加(校正p < 0.1),提示呼吸道纤毛丰度相对增加。
转录组分析表明,iSGS复发率较低与呼吸道纤毛保留有关,而复发率较高者存在适应性免疫反应和细胞外基质沉积增加。这些结果为开发iSGS的预后标志物和确定治疗靶点带来了希望。
