Intravacc (Institute for Translational Vaccinology), Bilthoven, Netherlands.
Centre for Health Protection, National Institute for Public Health and the Environment, Bilthoven, Netherlands.
Front Immunol. 2019 Jun 17;10:1364. doi: 10.3389/fimmu.2019.01364. eCollection 2019.
resurgence affects not only the unvaccinated, but also the vaccinated population. Different vaccines are available, however, it is currently unknown whether the type of childhood vaccination has an influence on antibody responses following a infection later in life. Therefore, the study aim was to profile serum antibody responses in young adults with suspected infections, immunized during childhood with either whole-cell (wPV) or monocomponent acellular pertussis (aPV) vaccines. Serum anti-pertussis toxin (PTx) IgG antibody levels served as an indicator for a recent infection. Leftover sera from a diagnostic laboratory from 36 Danish individuals were included and divided into four groups based on immunization background (aPV . wPV) and serum anti-PTx IgG levels (- . +). Pertussis-specific IgG/IgA antibody levels and antigen specificity were determined by using multiplex immunoassays (MIA), one- and two-dimensional immunoblotting (1 & 2DEWB), and mass spectrometry. Besides enhanced anti-PTx levels, wPV(+) and aPV(+) groups showed increased IgG and IgA levels against pertactin, filamentous hemagglutinin, fimbriae 2/3, and pertussis outer membrane vesicles (OMV). In the wPV(-) and aPV(-) groups, only low levels of anti-OMV antibodies were detected. 1DEWB demonstrated that antibody patterns differed between groups but also between individuals with the same immunization background and anti-PTx levels. 2DWB analysis for serum IgG revealed 133 immunogenic antigens of which 40 were significantly different between groups allowing to differentiate wPV(+) and aPV(+) groups. Similarly, for serum IgA, 7 of 47 immunogenic protein spots were significantly different. This study demonstrated that infection-induced antibody responses were distinct on antigen level between individuals with either wPV or aPV immunization background. Importantly, only 2DEWB and not MIA could detect these differences indicating the potential of this method. Moreover, in individuals immunized with an aPV containing only PTx in childhood, the infection-induced antibody responses were not limited to PTx alone.
再现不仅影响未接种疫苗的人群,也影响已接种疫苗的人群。目前有不同类型的疫苗可供选择,但尚不清楚儿童时期接种全细胞(wPV)还是单价组分无细胞百日咳(aPV)疫苗是否会影响成年后感染后的抗体反应。因此,本研究旨在分析疑似百日咳感染的年轻成年人的血清抗体反应,这些成年人在儿童时期接受过全细胞(wPV)或单价组分无细胞百日咳(aPV)疫苗接种。血清抗百日咳毒素(PTx)IgG 抗体水平可作为近期百日咳感染的指标。研究纳入了丹麦一个诊断实验室的 36 份剩余血清,根据免疫背景(aPV 或 wPV)和血清抗-PTx IgG 水平将其分为 4 组(-或+)。使用多重免疫分析(MIA)、一维和二维免疫印迹(1 & 2DEWB)和质谱法测定百日咳特异性 IgG/IgA 抗体水平和抗原特异性。除了增强的抗-PTx 水平外,wPV(+)和 aPV(+)组对 pertactin、丝状血凝素、fimbriae 2/3 和百日咳外膜囊泡(OMV)的 IgG 和 IgA 水平也有所增加。在 wPV(-)和 aPV(-)组中,仅检测到低水平的抗-OMV 抗体。1DEWB 表明,抗体模式在组间存在差异,在具有相同免疫背景和抗-PTx 水平的个体间也存在差异。血清 IgG 的 2DWB 分析显示 133 个免疫原性抗原,其中 40 个在组间存在显著差异,可区分 wPV(+)和 aPV(+)组。同样,对于血清 IgA,47 个免疫原性蛋白斑点中有 7 个在组间存在显著差异。本研究表明,在具有 wPV 或 aPV 免疫背景的个体中,感染诱导的抗体反应在抗原水平上存在明显差异。重要的是,只有 2DEWB 而不是 MIA 可以检测到这些差异,表明该方法具有潜力。此外,在儿童时期仅接种含有 PTx 的 aPV 疫苗的个体中,感染诱导的抗体反应不仅局限于 PTx 本身。
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