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差异抗原呈递调节初次和二次流感病毒感染中CD8 + T细胞免疫显性的变化模式。

Differential antigen presentation regulates the changing patterns of CD8+ T cell immunodominance in primary and secondary influenza virus infections.

作者信息

Crowe Sherry R, Turner Stephen J, Miller Shannon C, Roberts Alan D, Rappolo Rachel A, Doherty Peter C, Ely Kenneth H, Woodland David L

机构信息

Trudeau Institute, P.O. Box 59, Saranac Lake, NY 12983, USA.

出版信息

J Exp Med. 2003 Aug 4;198(3):399-410. doi: 10.1084/jem.20022151. Epub 2003 Jul 28.

Abstract

The specificity of CD8+ T cell responses can vary dramatically between primary and secondary infections. For example, NP366-374/Db- and PA224-233/Db-specific CD8+ T cells respond in approximately equal numbers to a primary influenza virus infection in C57BL/6 mice, whereas NP366-374/Db-specific CD8+ T cells dominate the secondary response. To investigate the mechanisms underlying this changing pattern of immunodominance, we analyzed the role of antigen presentation in regulating the specificity of the T cell response. The data show that both dendritic and nondendritic cells are able to present the NP366-374/Db epitope, whereas only dendritic cells effectively present the PA224-233/Db epitope after influenza virus infection, both in vitro and in vivo. This difference in epitope expression favored the activation and expansion of NP366-374/Db-specific CD8+ memory T cells during secondary infection. The data also show that the immune response to influenza virus infection may involve T cells specific for epitopes, such as PA224-233/Db, that are poorly expressed at the site of infection. In this regard, vaccination with the PA224-233 peptide actually had a detrimental effect on the clearance of a subsequent influenza virus infection. Thus, differential antigen presentation impacts both the specificity of the T cell response and the efficacy of peptide-based vaccination strategies.

摘要

CD8+ T细胞反应的特异性在初次感染和二次感染之间可能有显著差异。例如,在C57BL/6小鼠中,针对NP366 - 374/Db和PA224 - 233/Db的特异性CD8+ T细胞在初次流感病毒感染时反应数量大致相等,而针对NP366 - 374/Db的特异性CD8+ T细胞在二次反应中占主导。为了研究这种免疫优势变化模式背后的机制,我们分析了抗原呈递在调节T细胞反应特异性中的作用。数据表明,树突状细胞和非树突状细胞都能够呈递NP366 - 374/Db表位,而在流感病毒感染后,无论是在体外还是体内,只有树突状细胞能有效地呈递PA224 - 233/Db表位。表位表达的这种差异有利于二次感染期间针对NP366 - 374/Db的特异性CD8+记忆T细胞的激活和扩增。数据还表明,对流感病毒感染的免疫反应可能涉及对在感染部位表达较差的表位(如PA224 - 233/Db)具有特异性的T细胞。在这方面,用PA224 - 233肽进行疫苗接种实际上对随后流感病毒感染的清除有不利影响。因此,差异抗原呈递既影响T细胞反应的特异性,也影响基于肽的疫苗接种策略的效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c355/2194086/39f58ebdd62c/20022151f1.jpg

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