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流感病毒感染的免疫反应。

Immune responses to influenza virus infection.

机构信息

Department of Virology, Erasmus MC, Rotterdam, The Netherlands.

出版信息

Virus Res. 2011 Dec;162(1-2):19-30. doi: 10.1016/j.virusres.2011.09.022. Epub 2011 Sep 22.

DOI:10.1016/j.virusres.2011.09.022
PMID:21963677
Abstract

Influenza viruses cause annual outbreaks of respiratory tract infection with attack rates of 5-10%. This means that humans are infected repeatedly with intervals of, on average, 10-20 years. Upon each infection subjects develop innate and adaptive immune responses which aim at clearing the infection. Strain-specific antibody responses are induced, which exert selective pressure on circulating influenza viruses and which drive antigenic drift of seasonal influenza viruses, especially in the hemagglutinin molecule. This antigenic drift necessitates updating of seasonal influenza vaccines regularly in order to match the circulating strains. Upon infection also virus-specific T cell responses are induced, including CD4+ T helper cells and CD8+ cytotoxic T cells. These cells are mainly directed to conserved proteins and therefore display cross-reactivity with a variety of influenza A viruses of different subtypes. T cell mediated immunity therefore may contribute to so-called heterosubtypic immunity and may afford protection against antigenically distinct, potentially pandemic influenza viruses. At present, novel viral targets are identified that may help to develop broad-protective vaccines. Here we review the various arms of the immune response to influenza virus infections and their viral targets and discuss the possibility of developing universal vaccines. The development of such novel vaccines would imply that also new immune correlates of protection need to be established in order to facilitate assessment of vaccine efficacy.

摘要

流感病毒每年都会引起呼吸道感染的爆发,发病率为 5-10%。这意味着人类平均每 10-20 年会被重复感染一次。在每次感染中,宿主都会产生先天和适应性免疫反应,旨在清除感染。诱导产生针对特定毒株的抗体反应,对流行的流感病毒施加选择压力,驱动季节性流感病毒的抗原漂移,特别是在血凝素分子上。这种抗原漂移需要定期更新季节性流感疫苗,以匹配循环毒株。感染还会诱导针对病毒的 T 细胞反应,包括 CD4+辅助性 T 细胞和 CD8+细胞毒性 T 细胞。这些细胞主要针对保守蛋白,因此与不同亚型的多种流感 A 病毒具有交叉反应性。因此,T 细胞介导的免疫可能有助于所谓的异源免疫,并可能提供针对抗原不同、具有潜在大流行风险的流感病毒的保护。目前,已经确定了新的病毒靶点,这可能有助于开发广泛保护的疫苗。本文综述了针对流感病毒感染的免疫反应的各个方面及其病毒靶点,并讨论了开发通用疫苗的可能性。新型疫苗的开发意味着也需要建立新的免疫保护相关指标,以促进疫苗效果的评估。

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