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白细胞介素-17 依赖性分泌型免疫球蛋白 A 通过减毒活疫苗 BPZE1 对鼻博德特氏菌百日咳感染的保护作用。

IL-17-dependent SIgA-mediated protection against nasal Bordetella pertussis infection by live attenuated BPZE1 vaccine.

机构信息

Center of Infection and Immunity of Lille, Institut Pasteur de Lille, 59019, Lille, France.

Inserm U1019, 59019, Lille, France.

出版信息

Mucosal Immunol. 2018 Nov;11(6):1753-1762. doi: 10.1038/s41385-018-0073-9. Epub 2018 Aug 16.

DOI:10.1038/s41385-018-0073-9
PMID:30115992
Abstract

BPZE1 is a live attenuated Bordetella pertussis vaccine for nasal administration to mimic the natural route of infection. Here, we studied the mechanism of BPZE1-induced immunity in the murine nasal cavity in contrast to acellular vaccine (aPV), although both vaccines protected against lung colonization. Transfer of splenocytes or serum from BPZE1-vaccinated or aPV-vaccinated mice protected naïve mice against lung colonization but not against nasal colonization. However, transfer of nasal washes from BPZE1-vaccinated mice resulted in protection against nasal colonization, which was lost in IgA-deficient or poly-Ig receptor-deficient mice, indicating that it depends on secretory IgA (SIgA) induction induced in the nose. BPZE1-induced protection against nasal colonization was long-lived despite the relatively rapid decay of SIgA, indicating a potent BPZE1-induced local memory response, likely due to CD4 tissue-resident memory T cells induced in the nose by BPZE1. These cells produced interleukin-17 (IL-17), known to be important for SIgA secretion. Furthermore, BPZE1 failed to protect Il17 mice against nasal colonization by B. pertussis and induced only background levels of nasal SIgA. Thus, our results show important differences in the protective mechanism between the upper and the lower murine respiratory tract and demonstrate an IL-17-dependent SIgA-mediated mechanism of BPZE1-induced protection against B. pertussis nasopharyngeal colonization.

摘要

BPZE1 是一种经鼻内给药的减毒百日咳博德特氏菌活疫苗,旨在模拟自然感染途径。在这里,我们研究了 BPZE1 在小鼠鼻腔中诱导免疫的机制,与无细胞疫苗(aPV)形成对比,尽管这两种疫苗都能预防肺部定植。BPZE1 疫苗或 aPV 疫苗接种小鼠的脾细胞或血清转移可保护未感染小鼠免受肺部定植,但不能免受鼻腔定植。然而,BPZE1 疫苗接种小鼠的鼻腔冲洗液转移导致对鼻腔定植的保护,而在 IgA 缺陷或多 Ig 受体缺陷小鼠中则失去保护作用,表明这依赖于鼻腔中诱导的分泌型 IgA(SIgA)。尽管 SIgA 迅速衰减,但 BPZE1 诱导的鼻腔定植保护作用持久,表明 BPZE1 诱导了强大的局部记忆反应,可能是由于 BPZE1 在鼻腔中诱导了 CD4 组织驻留记忆 T 细胞。这些细胞产生白细胞介素 17(IL-17),已知其对 SIgA 分泌很重要。此外,BPZE1 不能保护 Il17 小鼠免受百日咳博德特氏菌的鼻腔定植,并且仅诱导背景水平的鼻腔 SIgA。因此,我们的研究结果表明,上呼吸道和下呼吸道的保护机制存在重要差异,并证明了 IL-17 依赖性 SIgA 介导的 BPZE1 诱导对百日咳博德特氏菌鼻咽定植的保护机制。

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