在呼吸道合胞病毒疫苗增强疾病的小鼠模型中,早期反应性CD8(+)记忆T细胞可减轻肺部嗜酸性粒细胞增多。
Pulmonary eosinophilia is attenuated by early responding CD8(+) memory T cells in a murine model of RSV vaccine-enhanced disease.
作者信息
Stevens Whitney W, Sun Jie, Castillo Jonathan P, Braciale Thomas J
机构信息
Beirne B. Carter Center for Immunology Research, University of Virginia, Charlottesville, Virginia 22908, USA.
出版信息
Viral Immunol. 2009 Jul;22(4):243-51. doi: 10.1089/vim.2009.0016.
Vaccination with formalin-inactivated respiratory syncytial virus (RSV) vaccine results in enhanced respiratory tract inflammation and injury following subsequent RSV infection. RSV vaccine-enhanced disease can also be produced in mice by prior vaccination with a vaccinia virus vector containing the RSV G protein, followed by intranasal infectious RSV challenge, a process characterized by induction of a potent memory CD4(+) T-cell response to challenge infection with some features characteristic of Th-2 CD4(+) T-cell responses, including increased eosinophil accumulation in pulmonary inflammatory infiltrates. The adaptive immune response to the RSV G protein in immunized BALB/c mice is characterized by a weak or absent primary and secondary recall CD8(+) T-cell response. These and related results have led to the hypothesis that the failure of the infected animals to mount an effective CD8(+) memory T-cell (CD8(+) Tm) response in this model could account for the pulmonary eosinophilia associated with the development of enhanced disease, and that CD8(+) T cells may control the development of eosinophilia. In this study, we investigated how and when the generation of a CD8(+) Tm response to RSV infection might affect the development of pulmonary eosinophilia in this model of vaccine-enhanced disease. By defining the CD8(+) T-cell response kinetics and monitoring lung parenchymal eosinophil accumulation, we show that the establishment of an RSV-specific CD8(+) Tm response in the infected lungs early after challenge infection (i.e., within the first 3 d of RSV infection) is necessary and sufficient to control pulmonary eosinophilia development. Additionally, our work suggests that the mechanism by which CD8(+) T cells regulate this process is not by modulating the differentiation or development of the CD4(+) Tm response. Rather, we demonstrate that IL-10 produced by early responding CD8(+) Tm cells may regulate the pulmonary eosinophilia development observed in RSV vaccine-enhanced disease.
用福尔马林灭活的呼吸道合胞病毒(RSV)疫苗进行接种,会导致后续RSV感染后呼吸道炎症和损伤加剧。用含有RSV G蛋白的痘苗病毒载体预先接种小鼠,随后进行鼻内感染性RSV攻击,也可产生RSV疫苗增强疾病,该过程的特征是诱导对攻击感染产生强大的记忆CD4(+) T细胞反应,具有一些Th-2 CD4(+) T细胞反应的特征,包括肺部炎性浸润中嗜酸性粒细胞积聚增加。免疫的BALB/c小鼠对RSV G蛋白的适应性免疫反应的特征是初次和二次回忆CD8(+) T细胞反应微弱或缺失。这些及相关结果导致了这样一种假说:在该模型中,受感染动物未能产生有效的CD8(+)记忆T细胞(CD8(+) Tm)反应,可能是与增强疾病发展相关的肺部嗜酸性粒细胞增多的原因,并且CD8(+) T细胞可能控制嗜酸性粒细胞增多的发展。在本研究中,我们调查了对RSV感染产生CD8(+) Tm反应的方式和时间,可能如何影响该疫苗增强疾病模型中肺部嗜酸性粒细胞增多的发展。通过确定CD8(+) T细胞反应动力学并监测肺实质嗜酸性粒细胞积聚,我们表明在攻击感染后早期(即RSV感染的前3天内)在受感染的肺部建立RSV特异性CD8(+) Tm反应,对于控制肺部嗜酸性粒细胞增多的发展是必要且充分的。此外,我们的工作表明,CD8(+) T细胞调节这一过程的机制不是通过调节CD4(+) Tm反应的分化或发育。相反,我们证明早期反应的CD8(+) Tm细胞产生的IL-10可能调节RSV疫苗增强疾病中观察到的肺部嗜酸性粒细胞增多的发展。
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