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Cross-Lineage Influenza B and Heterologous Influenza A Antibody Responses in Vaccinated Mice: Immunologic Interactions and B/Yamagata Dominance

机译:接种小鼠的跨谱系乙型流感和甲型异源流感抗体反应:免疫相互作用和B /山形优势。

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摘要

The annually reformulated trivalent inactivated influenza vaccine (TIV) includes both influenza A/subtypes (H3N2 and H1N1) but only one of two influenza B/lineages (Yamagata or Victoria). In a recent series of clinical trials to evaluate prime-boost response across influenza B/lineages, influenza-naïve infants and toddlers originally primed with two doses of 2008–09 B/Yamagata-containing TIV were assessed after two doses of B/Victoria-containing TIV administered in the subsequent 2009–10 and 2010–11 seasons. In these children, the Victoria-containing vaccines strongly recalled antibody to the initiating B/Yamagata antigen but induced only low B/Victoria antibody responses. To further evaluate this unexpected pattern of cross-lineage vaccine responses, we conducted additional immunogenicity assessment in mice. In the current study, mice were primed with two doses of 2008–09 Yamagata-containing TIV and subsequently boosted with two doses of 2010–11 Victoria-containing TIV (Group-Yam/Vic). With the same vaccines, we also assessed the reverse order of two-dose Victoria followed by two-dose Yamagata immunization (Group-Vic/Yam). The Group-Yam/Vic mice showed strong homologous responses to Yamagata antigen. However, as previously reported in children, subsequent doses of Victoria antigen substantially boosted Yamagata but induced only low antibody response to the immunizing Victoria component. The reverse order of Group-Vic/Yam mice also showed low homologous responses to Victoria but subsequent heterologous immunization with even a single dose of Yamagata antigen induced substantial boost response to both lineages. For influenza A/H3N2, homologous responses were comparably robust for the differing TIV variants and even a single follow-up dose of the heterologous strain, regardless of vaccine sequence, substantially boosted antibody to both strains. For H1N1, two doses of 2008–09 seasonal antigen significantly blunted response to two doses of the 2010–11 pandemic H1N1 antigen. Immunologic interactions between influenza viruses considered antigenically distant and in particular the cross-lineage influenza B and dominant Yamagata boost responses we have observed in both human and animal studies warrant further evaluation.
机译:每年重新制定的三价灭活流感疫苗(TIV)包括两种甲型流感/亚型(H3N2和H1N1),但仅包括两种乙型流感/谱系(山形或维多利亚)中的一种。在最近的一系列临床试验中,评估了各种B型流感/血统的初免-加强反应,在两剂B / Victoria-H2疫苗接种后,最初接种了两剂2008–09 B / Yamagata的TIV初次接种流感的初生婴儿和幼儿。包含在随后的2009-10和2010-11赛季中施用的TIV。在这些儿童中,含维多利亚的疫苗强烈回忆起针对起始B / Yamagata抗原的抗体,但仅诱导了低B / Victoria抗体反应。为了进一步评估这种跨谱系疫苗反应的意外模式,我们在小鼠中进行了额外的免疫原性评估。在当前的研究中,小鼠接受了两剂2008–09年山形的TIV的灌注,然后接受了两剂2010–11维多利亚州的TIV(Group-Yam / Vic)加强免疫。使用相同的疫苗,我们还评估了两剂维多利亚疫苗的反向顺序,然后进行了两剂山形疫苗的免疫(Group-Vic / Yam)。 Group-Yam / Vic小鼠显示出对Yamagata抗原的强烈同源反应。然而,如先前在儿童中报道的,随后剂量的维多利亚抗原显着增强了山形,但仅诱导了对免疫维多利亚成分的低抗体应答。相反,Group-Vic / Yam小鼠的顺序也显示出对维多利亚的低同源性应答,但随后甚至用单剂量的Yamagata抗原进行的异源免疫也引起了对两种谱系的实质性增强应答。对于A / H3N2流感,对于不同的TIV变体,同源反应相当强大,即使是单一后续剂量的异源菌株,无论疫苗序列如何,都可以显着增强针对这两种菌株的抗体。对于H1N1,两剂2008–09季节性抗原显着减弱了对两剂2010–11大流行H1N1抗原的反应。我们在人类和动物研究中都观察到,在抗原上距离遥远的流感病毒,特别是跨谱系的B型流感和主要的Yamagata增强反应之间的免疫学相互作用值得进一步评估。

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