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Dynamics of IFN-β Responses during Respiratory Viral Infection. Insights for Therapeutic Strategies

免疫学 医学 慢性阻塞性肺病 细胞因子 先天免疫系统 免疫系统 病毒载量 流式细胞术 单反病毒 哮喘 病毒 病毒性疾病 副粘病毒科 内科学
作者
Alastair Watson,C. Mirella Spalluto,Christopher McCrae,Doriana Cellura,Hannah Burke,Danen Cunoosamy,Anna Freeman,Alex Hicks,Michael Hühn,Kristoffer Ostridge,Karl J. Staples,Outi Vaarala,Tom Wilkinson
出处
期刊:American Journal of Respiratory and Critical Care Medicine [American Thoracic Society]
卷期号:201 (1): 83-94 被引量:60
标识
DOI:10.1164/rccm.201901-0214oc
摘要

Rationale: Viral infections are major drivers of exacerbations and clinical burden in patients with asthma and chronic obstructive pulmonary disease (COPD). IFN-β is a key component of the innate immune response to viral infection. To date, studies of inhaled IFN-β treatment have not demonstrated a significant effect on asthma exacerbations.Objectives: The dynamics of exogenous IFN-β activity were investigated to inform on future clinical indications for this potential antiviral therapy.Methods: Monocyte-derived macrophages (MDMs), alveolar macrophages, and primary bronchial epithelial cells (PBECs) were isolated from healthy control subjects and patients with COPD and infected with influenza virus either prior to or after IFN-β stimulation. Infection levels were measured by the percentage of nucleoprotein 1-positive cells using flow cytometry. Viral RNA shedding and IFN-stimulated gene expression were measured by quantitative PCR. Production of inflammatory cytokines was measured using MSD.Measurements and Main Results: Adding IFN-β to MDMs, alveolar macrophages, and PBECs prior to, but not after, infection reduced the percentage of nucleoprotein 1-positive cells by 85, 56, and 66%, respectively (P < 0.05). Inhibition of infection lasted for 24 hours after removal of IFN-β and was maintained albeit reduced up to 1 week in MDMs and 72 hours in PBECs; this was similar between healthy control subjects and patients with COPD. IFN-β did not induce inflammatory cytokine production by MDMs or PBECs but reduced influenza-induced IL-1β production by PBECs.Conclusions:In vitro modeling of IFN-β dynamics highlights the potential for intermittent prophylactic doses of exogenous IFN-β to modulate viral infection. This provides important insights to aid the future design of clinical trials of IFN-β in asthma and COPD.
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