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Inactivated influenza vaccine adjuvanted with Bacterium-like particles induce systemic and mucosal influenza A virus specific T-cell and B-cell responses after nasal administration in a TLR2 dependent fashion

机译:佐有细菌样颗粒的灭活流感疫苗以TLR2依赖性方式经鼻给药后诱导全身和粘膜A型流感病毒特异性T细胞和B细胞反应

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摘要

Background: Nasal vaccination is considered to be a promising alternative for parenteral vaccination against influenza virus as it is non-invasive and offers the opportunity to elicit strong antigen-specific responses both systemic and locally at the port of entry of the pathogen. Previous studies showed that non-living bacterium-like particles (BLPs) from the food-grade bacterium Lactococcus lact-is are effective stimulators of local and systemic immune responses when administered intranasally. Moreover, in vitro, BLPs specifically interact with human Toll-like receptor 2 (TLR2), suggestive of a role for TLR2 dependent immune activation by BLPs. Methods: In the present study, we examined the role of TLR2 in vivo in immune activation after nasal administration of BLP mixed with split influenza vaccine (BLP-SV) of influenza A virus (IAV) using TLR2 knockout mice. Results: The systemic Th1 cell and subsequent B-cell responses induced after intranasal BLP-SV vaccination depended on the interaction of BLPs with TLR2. Notably, the BLP-SV-induced class switch to IgG2c depended on the interaction of BLP with TLR2. Local induced IAV-specific Th1 cell responses and the mucosal B-cell responses also depended on interaction of BLP with TLR2. Strongly reduced SIgA levels were observed in TLR2 knockout mice both in the nasal and vaginal lavages. In addition, detailed analysis of the T-cell response revealed that nasal BLP-SV vaccination promoted Th1/Th17 immune responses that coincided with increased IAV-specific IgG2c antibody production. Discussion: Altogether these results indicate that nasal BLP-SV vaccination induces IAV-specific T-cell and B-cell responses, both systemically and at the site of virus entry in a TLR2-dependent manner. (C) 2014 The Authors. Published by Elsevier Ltd.
机译:背景:鼻疫苗被认为是针对流感病毒的肠胃外疫苗的一种有前途的替代方法,因为它是非侵入性的,并提供了在病原体进入口引发全身和局部强烈抗原特异性反应的机会。以前的研究表明,鼻内给药时,食品级细菌乳酸乳球菌的非活菌样颗粒(BLP)是有效的局部和全身免疫应答刺激剂。此外,在体外,BLP与人Toll样受体2(TLR2)特异性相互作用,提示BLP对TLR2依赖性免疫激活具有作用。方法:在本研究中,我们使用TLR2基因敲除小鼠,对鼻腔施用BLP混合甲型流感病毒(IAV)的流感分裂疫苗(BLP-SV)混合后的体内TLR2在免疫激活中的作用进行了研究。结果:鼻内BLP-SV疫苗接种后诱导的全身Th1细胞和随后的B细胞反应取决于BLP与TLR2的相互作用。值得注意的是,BLP-SV诱导的向IgG2c的类别转换取决于BLP与TLR2的相互作用。局部诱导的IAV特异性Th1细胞反应和粘膜B细胞反应也取决于BLP与TLR2的相互作用。在TLR2基因敲除小鼠的鼻腔和阴道灌洗液中均观察到SIgA含量大大降低。此外,对T细胞应答的详细分析显示,鼻腔BLP-SV疫苗接种可促进Th1 / Th17免疫应答,这与IAV特异性IgG2c抗体产生的增加同时发生。讨论:总而言之,这些结果表明,鼻腔BLP-SV疫苗接种会全身性地以及在病毒进入部位以TLR2依赖性方式诱导IAV特异性T细胞和B细胞反应。 (C)2014作者。由Elsevier Ltd.发布

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