甲型干扰素预处理可减轻流感病毒感染诱导人鼻息肉上皮细胞中白细胞介素-25的表达。
Induction of IL-25 Expression in Human Nasal Polyp Epithelium by Influenza Virus Infection is Abated by Interferon-Alpha Pretreatment.
作者信息
Hong Haiyu, Tan Kai Sen, Yan Yan, Chen Fenghong, Ong Hsiao Hui, Oo Yukei, Liu Jing, Ong Yew Kwang, Thong Mark, Sugrue Richard, Chow Vincent T, Wang De Yun
机构信息
Allergy Center, Department of Otolaryngology, The Fifth Affiliated Hospital of Sun Yat-sen University, Zhuhai, People's Republic of China.
Otorhinolaryngology Hospital, The First Affiliated Hospital of Sun Yat-sen University, Guangzhou, People's Republic of China.
出版信息
J Inflamm Res. 2021 Jun 28;14:2769-2780. doi: 10.2147/JIR.S304320. eCollection 2021.
BACKGROUND
Epithelial cytokines including IL-25, IL-33 and thymic stromal lymphopoietin (TLSP) are recently established as drivers of type 2 chronic inflammatory diseases such as chronic rhinosinusitis with nasal polyps (CRSwNP). Here, we further confirmed the increased expression of IL-25 in CRSwNP and investigated potential contributors of IL-25 in CRSwNP epithelium.
METHODS
Sixty CRSwNP, 25 CRSsNP and 15 healthy control tissues were examined for IL-25 expression and for the accompanying type 2 inflammatory cytokines. We then tested different respiratory virus infections on human nasal epithelial cells (hNECs) for their ability to trigger IL-25 expression. In addition, we subjected hNECs generated from CRSwNP tissues to pretreatment with recombinant interferon-alpha (IFN-α) prior to viral infection to evaluate IFN effects on IL-25 induction.
RESULTS
We confirmed that significantly enhanced levels of IL-25 were observed in CRSwNP tissues, and that IL-25 expression correlated with type 2 inflammatory cytokine expression. In vitro, we observed significantly elevated IL-25 in hNECs infected with influenza A virus as early as 24 hours post-infection (hpi), regardless of tissue origin, and IL-25 correlated positively with viral load. While other respiratory viruses exhibited increasing trends of IL-25, these were not significant at the time-points tested. IFN-α treatment of CRSwNP epithelium was found to exert bimodal effects, ie IFN-α treatment alone induced moderate IL-25 expression, whereas IFN-α pretreatment of hNECs before influenza infection significantly diminished IL-25 induction by active influenza virus infection.
CONCLUSION
We have authenticated the observation of elevated IL-25 in CRSwNP, which is correlated with type 2 inflammatory cytokines. Notably, we identified influenza virus infection as a potential contributor of IL-25 in both control and CRSwNP epithelium during active infection. This IL-25 induction can be abated by IFN-α pretreatment which ameliorated active influenza infection.
TRIAL REGISTRATION
Chictr.org.cn ChiCTR-BON-16010179, Registered 18 December 2016, http://www.chictr.org.cn/showproj.aspx?proj=17331. The authors agree on the sharing of deidentified participant data where it pertains to request directly related to the data in this article when contacted (Haiyu Hong; honghy@mail.sysu.edu.cn).
背景
上皮细胞因子包括白细胞介素-25(IL-25)、白细胞介素-33(IL-33)和胸腺基质淋巴细胞生成素(TSLP),最近被确定为2型慢性炎症性疾病(如伴鼻息肉的慢性鼻-鼻窦炎,CRSwNP)的驱动因素。在此,我们进一步证实了IL-25在CRSwNP中的表达增加,并研究了CRSwNP上皮中IL-25的潜在促成因素。
方法
对60例CRSwNP、25例CRSsNP和15例健康对照组织进行IL-25表达及相关2型炎症细胞因子的检测。然后,我们检测了不同呼吸道病毒感染人鼻上皮细胞(hNECs)触发IL-25表达的能力。此外,我们对来自CRSwNP组织的hNECs在病毒感染前用重组干扰素-α(IFN-α)进行预处理,以评估IFN对IL-25诱导的影响。
结果
我们证实CRSwNP组织中IL-25水平显著升高,且IL-25表达与2型炎症细胞因子表达相关。在体外,我们观察到感染甲型流感病毒的hNECs在感染后24小时(hpi)就有显著升高的IL-25,无论组织来源如何,且IL-25与病毒载量呈正相关。虽然其他呼吸道病毒也呈现IL-25升高趋势,但在检测时间点上不显著。发现IFN-α处理CRSwNP上皮具有双峰效应,即单独的IFN-α处理诱导适度的IL-25表达,而在流感感染前对hNECs进行IFN-α预处理显著减少了活性流感病毒感染诱导的IL-25。
结论
我们证实了CRSwNP中IL-25升高的观察结果,其与2型炎症细胞因子相关。值得注意的是,我们确定在活跃感染期间,流感病毒感染是对照和CRSwNP上皮中IL-25的潜在促成因素。这种IL-25诱导可通过IFN-α预处理减轻,IFN-α预处理改善了活性流感感染。
试验注册
中国临床试验注册中心ChiCTR-BON-16010179,于2016年12月18日注册,http://www.chictr.org.cn/showproj.aspx?proj=17331。作者同意在被联系(洪海钰;honghy@mail.sysu.edu.cn)时共享与本文数据直接相关的去识别化参与者数据。
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