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干扰素-β在流感病毒感染期间调节 1 型免疫。

Interferon-β modulates type 1 immunity during influenza virus infection.

机构信息

Department of Immunology, University of Toronto, Toronto, Ontario M5S 1A8, Canada.

出版信息

Antiviral Res. 2010 Oct;88(1):64-71. doi: 10.1016/j.antiviral.2010.07.006. Epub 2010 Jul 24.

Abstract

Influenza viruses are important human pathogens, associated throughout history with worldwide outbreaks and pandemics. The antiviral effects of interferon (IFN)-αs/β against influenza virus infections are well recognized, yet the mechanisms whereby IFNs exert their immunomodulatory effects on an anti-influenza response remain ill-defined. Here, we describe the effects of IFN-β treatment on the immune response during a respiratory influenza (A/WSN/33) A virus infection of mice. A single dose of IFN-β (1×10(5)U) enhanced DC migration into the draining lymph node (DLN) on day 3 post-intranasal infection, and subsequently inhibited the migration from the lungs into the DLN of a newly identified late activator antigen-presenting cell population associated with type 2 immunity, LAPC. IFN-β treatment polarized the immune response towards a type 1 immune response, eliciting enhanced T(H)1 effector and cytolytic T cell responses, but diminished T(H)2 effector T cell responses in both the DLN and lung tissues of influenza virus-infected mice. Associated with the polarization towards a type 1 immune response, IFN-β treatment of mice resulted in accelerated viral clearance and diminished pulmonary eosinophilia in infected lung tissues.

摘要

流感病毒是重要的人类病原体,与历史上的全球爆发和大流行有关。干扰素(IFN)-α/β对流感病毒感染的抗病毒作用已得到广泛认可,但 IFN 发挥其免疫调节作用对抗流感反应的机制仍不清楚。在这里,我们描述了 IFN-β 处理对呼吸道流感(A/WSN/33)A 病毒感染小鼠免疫反应的影响。单次 IFN-β(1×10(5)U)处理可增强病毒感染后第 3 天进入引流淋巴结(DLN)的 DC 迁移,随后抑制与 2 型免疫相关的新鉴定的晚期激活抗原呈递细胞群(LAPC)从肺部进入 DLN 的迁移。IFN-β 处理将免疫反应向 1 型免疫反应极化,引发增强的 T(H)1 效应和细胞毒性 T 细胞反应,但在流感病毒感染小鼠的 DLN 和肺部组织中减弱 T(H)2 效应 T 细胞反应。与向 1 型免疫反应的极化相关,IFN-β 处理可加速病毒清除并减少感染肺部组织中的嗜酸性粒细胞。

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