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Role of innate lymphoid cells and dendritic cells in intradermal immunization of the enterovirus antigen

机译:先天淋巴细胞和树突细胞在肠道病毒抗原皮内免疫的作用

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Enterovirus type 71 (EV71) and coxsackievirus A 16 (CA16) are the major pathogens of human hand, foot, and mouth disease (HFMD). In our previous study, intramuscular immunization with the inactivated EV71 vaccine elicited effective immunity, while immunization with the inactivated CA16 vaccine did not. In this report, we focused on innate immune responses elicited by inactivated EV71 and CA16 antigens administered intradermally or intramuscularly. The distributions of the EV71 and CA16 antigens administered intradermally or intramuscularly were not obviously different, but the antigens were detected for a shorter period of time when administered intradermally. The expression levels of NF-κB pathway signaling molecules, which were identified as being capable of activating DCs, ILCs, and T cells, were higher in the intradermal group than in the intramuscular group. Antibodies for the EV71 and CA16 antigens colocalized with ILCs and DCs in skin and muscle tissues under fluorescence microscopy. Interestingly, ILC colocalization decreased over time, while DC colocalization increased over time. ELISpot analysis showed that coordination between DCs and ILCs contributed to successful adaptive immunity against vaccine antigens in the skin. EV71 and/or CA16 antigen immunization via the intradermal route was more capable of significantly increasing neutralizing antibody titers and activating specific T cell responses than immunization via the intramuscular route. Furthermore, neonatal mice born to mothers immunized with the EV71 and CA16 antigens were 100% protected against wild-type EV71 or CA16 viral challenge. Together, our results provide new insights into the development of vaccines for HFMD.
机译:肠道病毒类型71(EV71)和Coxsackievirus A 16(Ca16)是人手,脚和口病(HFMD)的主要病原体。在我们以前的研究中,用灭活的EV71疫苗引起有效免疫的肌肉内免疫,同时用灭活的Ca16疫苗免疫没有。在本报告中,我们专注于灭活的EV71和CA16抗原引发的先天免疫应答,或肌肉内施用。 eV71和Ca16抗原的分布在皮内或肌肉内施用,未明显不同,但在皮内给药时检测抗原较短的时间。 NF-κB途径信号分子的表达水平被鉴定为能够激活DCS,ILC和T细胞,在皮内组中较高,而不是肌内组。 EV71和Ca16抗原的抗体在荧光显微镜下用ILC和肌肉组织中的ILC和DC分致大致聚集。有趣的是,ILC Colocalization随着时间的推移而降低,而DC Colocalization随着时间的推移而增加。 ELISPOT分析表明,DCS和ILC之间的协调有助于成功对皮肤疫苗抗原的适应性免疫。通过皮内途径的EV71和/或Ca16抗原免疫,更能显着增加中和抗体滴度,并使比通过肌内途径免疫的特异性T细胞应答。此外,对与EV71和Ca16抗原免疫的母亲出生的新生小鼠100%免受野生型EV71或Ca16病毒攻击。我们的结果在一起,为HFMD的疫苗开发提供了新的见解。

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