Subcutaneous immunisation with zymosan generates mucosal IgA-eliciting memory and protects mice from heterologous influenza virus infection.

IF 4.8 4区 医学 Q2 IMMUNOLOGY International immunology Pub Date : 2023-08-07 DOI:10.1093/intimm/dxad013
Yoshihito Nihei, Mizuki Higashiyama, Kosuke Miyauchi, Kei Haniuda, Yusuke Suzuki, Masato Kubo, Daisuke Kitamura
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Abstract

Immunoglobulin A (IgA) is the most abundant isotype of antibodies and provides a first line of defense at the mucosa against pathogens invading the host. It has been widely accepted that the mucosal IgA response provided by vaccination requires mucosal inoculation, and intranasal inoculation has been proposed for vaccines against influenza virus. Considering the difficulty of intranasal vaccination in infants or elderly people, however, parenteral vaccination that provides the mucosal IgA response is desirable. Here, we demonstrate that subcutaneous immunisation with zymosan, a yeast cell wall constituent known to be recognised by Dectin-1 and TLR2, potentiates the production of antigen-specific IgA antibodies in the sera and airway mucosa upon intranasal antigen challenge. We confirmed that the antigen-specific IgA-secreting cells accumulated in the lung and nasal-associated lymphoid tissues after the antigen challenge. Such an adjuvant effect of zymosan in the primary immunisation for the IgA response depended on Dectin-1 signalling, but not on TLR2. The IgA response to the antigen challenge required both antigen-specific memory B and T cells, and the generation of memory T cells, but not memory B cells, depended on zymosan as an adjuvant. Finally, we demonstrated that subcutaneous inoculation of inactivated influenza virus with zymosan, but not with alum, mostly protected the mice from infection with a lethal dose of a heterologous virus strain. These data suggest that zymosan is a possible adjuvant for parenteral immunisation that generates memory IgA responses to respiratory viruses such as influenza virus.

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用酶生酶皮下免疫产生粘膜iga诱导记忆并保护小鼠免受异源流感病毒感染。
免疫球蛋白A (IgA)是抗体中最丰富的同型抗体,为黏膜抵御病原体入侵提供了第一道防线。疫苗接种提供的粘膜IgA反应需要粘膜接种,已被广泛接受,流感病毒疫苗已被提出鼻内接种。然而,考虑到婴儿或老年人鼻内接种疫苗的困难,提供粘膜IgA反应的肠外接种是可取的。在本研究中,我们证明了用zymosan(一种已知可被Dectin-1和TLR2识别的酵母细胞壁成分)皮下免疫,在鼻内抗原攻击时,增强了血清和气道黏膜中抗原特异性IgA抗体的产生。我们证实抗原特异性iga分泌细胞在抗原激发后在肺和鼻相关淋巴组织中积累。zymosan在初次免疫中对IgA应答的辅助作用依赖于Dectin-1信号,而不依赖于TLR2。对抗原攻击的IgA反应需要抗原特异性记忆B细胞和T细胞,并且记忆T细胞的产生依赖于zymosan作为佐剂,而不是记忆B细胞。最后,我们证明了皮下接种灭活流感病毒的酶酶酶,而不是明矾,大多保护小鼠免受致命剂量的异源病毒株的感染。这些数据表明,zymosan可能是肠外免疫的辅助剂,可对呼吸道病毒(如流感病毒)产生记忆性IgA反应。
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来源期刊
International immunology
International immunology 医学-免疫学
CiteScore
9.30
自引率
2.30%
发文量
51
审稿时长
6-12 weeks
期刊介绍: International Immunology is an online only (from Jan 2018) journal that publishes basic research and clinical studies from all areas of immunology and includes research conducted in laboratories throughout the world.
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