Late response of bronchial epithelium to rhinovirus in severe asthma

IF 0.5 4区 医学 Q4 RESPIRATORY SYSTEM Revue des maladies respiratoires Pub Date : 2024-03-01 DOI:10.1016/j.rmr.2024.01.014
K. Valette , L. Moreno , A.S. Payet , P. Chanez , D. Gras
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Abstract

Introduction

Alteration of bronchial epithelium is one of the main features of severe asthma. Bronchial epithelial cells (BEC) promote airway inflammation and remodeling leading to chronic symptoms and airway hyperresponsiveness and obstruction. Moreover, BEC are the first line in viral infections, which are the major contributor to asthma exacerbation. However, the consequences of the persisting long-term responses to viral infection of BEC in severe asthma are not fully understood. The aim of our study was to investigate the morphological and functional responses of bronchial epithelium induced by human rhinovirus in acute and late phase post-infection in severe asthma in an ALI culture model.

Methods

Primary human bronchial epithelial cells (HBECs) from control (C) (n = 3) and severe asthmatic (SA) (n = 4), cultured in air–liquid interface (ALI), were infected with Rhinovirus A16 (RV-A16) at the apical pole. The virus was removed four hours after infection. Differences in term of viral replication, cytotoxicity (measured by LDH activity), epithelium cohesion (TEER measurement) and antiviral response was assessed at the acute phase (until 4 days) and at the late phase (until 14 days) post-infection (dpi).

Results

RV-A16 replication increased during the acute phase then decreased during the late phase, without difference between control and severe asthmatic. Cytotoxicity was slightly induced by RV-A16 infection only in the acute phase with no difference observed between control and severe asthmatic (fold induction compared to MOCK: 10.4 and 11.7 for C and SA respectively at 4 dpi). Epithelium cohesion is damaged by RV-A16 in severe asthmatics at the late phase whereas it is strengthened in controls (Fold induction compared to MOCK: 1.12 and 0.62 for C and SA respectively at 14 dpi). RV-A16 induced secretion of several antiviral defense peptides (IFNλ2-3, IFNλ1, IFNβ, IFNα2) and inflammatory mediators (CCL5, CXCL10, IL 33, TSLP) over the first week post-infection, with different kinetic and intensities between control and severe asthmatic. IL-33 and TSLP secretion is significantly more induced in severe asthmatic than in control (P < 0.05). Antiviral and proinflammatory mediator's secretion returns to baseline at 14 dpi in both severe asthmatics and controls, but declines more rapidly in severe asthmatics.

Conclusion

The antiviral response is different in terms of profile and intensity between control and severe asthmatic, both in the acute and late phases. The virus induces alteration of epithelium cohesion in severe asthmatics, suggesting a defect in cellular events normally induced by injury. Then, an altered response of HBECs in severe asthma, illustrated by the increased secretion of epithelial alarmins IL-33 and TSLP, could contribute to increased disease susceptibility and an enhanced inflammatory response to rhinovirus infection.

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严重哮喘患者支气管上皮细胞对鼻病毒的晚期反应
导言支气管上皮细胞的改变是严重哮喘的主要特征之一。支气管上皮细胞(BEC)促进气道炎症和重塑,导致慢性症状、气道高反应性和阻塞。此外,支气管上皮细胞是病毒感染的第一线,而病毒感染是导致哮喘恶化的主要因素。然而,BEC 对病毒感染的长期持续反应对重症哮喘的影响尚不完全清楚。我们研究的目的是在 ALI 培养模型中研究人鼻病毒感染重症哮喘患者急性期和晚期支气管上皮细胞后诱导的形态和功能反应。感染四小时后清除病毒。结果RV-A16的复制在急性期增加,在晚期减少,对照组和重症哮喘患者之间没有差异。RV-A16 感染仅在急性期对细胞毒性有轻微诱导作用,对照组和重度哮喘患者的细胞毒性没有差异(与 MOCK 相比,4 dpi 时 C 和 SA 的诱导倍数分别为 10.4 和 11.7)。在晚期阶段,RV-A16 会破坏严重哮喘患者上皮细胞的凝聚力,而在对照组中则会加强这种凝聚力(14 dpi 时,与 MOCK 相比,C 和 SA 的诱导倍数分别为 1.12 和 0.62)。在感染后的第一周,RV-A16 诱导了多种抗病毒防御肽(IFNλ2-3、IFNλ1、IFNβ、IFNα2)和炎症介质(CCL5、CXCL10、IL 33、TSLP)的分泌,对照组和重症哮喘患者分泌的动力学和强度不同。重症哮喘患者的 IL-33 和 TSLP 分泌明显高于对照组(P < 0.05)。严重哮喘患者和对照组的抗病毒和促炎介质分泌在 14 dpi 时均恢复到基线水平,但严重哮喘患者的下降速度更快。病毒会诱导重症哮喘患者上皮细胞内聚力的改变,这表明通常由损伤诱导的细胞事件存在缺陷。重症哮喘患者上皮警戒素 IL-33 和 TSLP 的分泌增加说明 HBECs 的反应发生了改变,这可能会导致对疾病的易感性增加以及对鼻病毒感染的炎症反应增强。
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来源期刊
Revue des maladies respiratoires
Revue des maladies respiratoires 医学-呼吸系统
CiteScore
1.10
自引率
16.70%
发文量
168
审稿时长
4-8 weeks
期刊介绍: La Revue des Maladies Respiratoires est l''organe officiel d''expression scientifique de la Société de Pneumologie de Langue Française (SPLF). Il s''agit d''un média professionnel francophone, à vocation internationale et accessible ici. La Revue des Maladies Respiratoires est un outil de formation professionnelle post-universitaire pour l''ensemble de la communauté pneumologique francophone. Elle publie sur son site différentes variétés d''articles scientifiques concernant la Pneumologie : - Editoriaux, - Articles originaux, - Revues générales, - Articles de synthèses, - Recommandations d''experts et textes de consensus, - Séries thématiques, - Cas cliniques, - Articles « images et diagnostics », - Fiches techniques, - Lettres à la rédaction.
期刊最新文献
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