Sauerhering Lucie, Müller Helena, Behner Laura, Elvert Mareike, Fehling Sarah Katharina, Strecker Thomas, Maisner Andrea
Institute of Virology, Philipps University Marburg, Marburg, Germany.
J Gen Virol. 2017 Oct;98(10):2447-2453. doi: 10.1099/jgv.0.000934. Epub 2017 Oct 6.
Highly pathogenic Nipah virus (NiV) generally causes severe encephalitis in humans. Respiratory symptoms are infrequently observed, likely reflecting variations in infection kinetics in human airways. Supporting this idea, we recently identified individual differences in NiV replication kinetics in cultured airway epithelia from different human donors. As type III interferons (IFN-λ) represent major players in the defence mechanism against viral infection of the respiratory mucosa, we studied IFN-λ induction and antiviral activity in NiV-infected primary differentiated human bronchial epithelial cells (HBEpCs) cultured under air-liquid interface conditions. Our studies revealed that IFN-λ was upregulated in airway epithelia upon NiV infection. We also show that IFN-λ pretreatment efficiently inhibited NiV replication. Interestingly, the antiviral activity of IFN-λ varied in HBEpCs from two different donors. Increased sensitivity to IFN-λ was associated with higher expression levels of IFN-λ receptors, enhanced phosphorylation of STAT1, as well as enhanced induction of interferon-stimulated gene expression. These findings suggest that individual variations in IFN-λ receptor expression affecting IFN responsiveness can play a functional role for NiV replication kinetics in human respiratory epithelial cells of different donors.
高致病性尼帕病毒(NiV)通常会导致人类严重脑炎。呼吸道症状并不常见,这可能反映了人类气道中感染动力学的差异。支持这一观点的是,我们最近在来自不同人类供体的培养气道上皮细胞中发现了NiV复制动力学的个体差异。由于III型干扰素(IFN-λ)是呼吸道黏膜抗病毒感染防御机制的主要参与者,我们研究了在气液界面条件下培养的NiV感染的原代分化人支气管上皮细胞(HBEpCs)中IFN-λ的诱导和抗病毒活性。我们的研究表明,NiV感染后气道上皮细胞中的IFN-λ上调。我们还表明,IFN-λ预处理能有效抑制NiV复制。有趣的是,来自两个不同供体的HBEpCs中IFN-λ的抗病毒活性有所不同。对IFN-λ敏感性的增加与IFN-λ受体的更高表达水平、STAT1的增强磷酸化以及干扰素刺激基因表达的增强诱导有关。这些发现表明,影响IFN反应性的IFN-λ受体表达的个体差异可能对不同供体的人呼吸道上皮细胞中NiV的复制动力学发挥功能性作用。
