首页> 外文OA文献 >Heterologous Prime-Boost Vaccination with MF59-Adjuvanted H5 Vaccines Promotes Antibody Affinity Maturation towards the Hemagglutinin HA1 Domain and Broad H5N1 Cross-Clade Neutralization
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Heterologous Prime-Boost Vaccination with MF59-Adjuvanted H5 Vaccines Promotes Antibody Affinity Maturation towards the Hemagglutinin HA1 Domain and Broad H5N1 Cross-Clade Neutralization

机译:MF59辅助H5疫苗的异源初免-加强疫苗可促进针对血凝素HA1域的抗体亲和力成熟和广泛的H5N1跨进化中和

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摘要

In an open label clinical study (2007), MF59-adjuvanted hemagglutinin (HA) vaccine from H5N1-A/Vietnam/1194/2004 (clade 1) was administered to subjects previously vaccinated (primed) with clade 0 H5N3 (A/duck/Singapore/97) vaccine at least 6 years earlier (in 1999 or 2001). The primed individuals responded rapidly and generated high neutralizing antibody titers against the H5N1-Vietnam strain within 7 days of a single booster vaccination. Furthermore, significant cross-neutralization titers were measured against H5N1 clade 0, 1, and 2 viruses. In the current study, the impact of MF59 adjuvant during heterologous priming on the quality of humoral polyclonal immune response in different vaccine arms were further evaluated using real time kinetics assay by surface plasmon resonance (SPR). Total anti-H5N1 HA1 polyclonal sera antibody binding from the heterologous prime-boost groups after a single MF59-H5N1 boost was significantly higher compared with sera from unprimed individuals that received two MF59-H5N1 vaccinations. The antigen-antibody complex dissociation rates (surrogate for antibody affinity) of the polyclonal sera against HA1 of H5N1-A/Vietnam/1194/2004 from the MF59-H5N3 primed groups were significantly higher compared to sera from unadjuvanted primed groups or unprimed individuals that received two MF59-H5N1 vaccines. Furthermore, strong inverse correlations were observed between the antibody dissociation off-rates of the immune sera against HA1 (but not HA2) and the virus neutralization titers against H5 vaccine strains and heterologous H5N1 strains. These findings supports the use of oil-in-water-adjuvanted pandemic influenza vaccines to elicit long term memory B cells with high affinity BCR capable of responding to potential variant pandemic viruses likely to emerge and adapt to human transmissions.
机译:在一项开放标签的临床研究(2007年)中,将H5N1-A /越南/ 1194/2004(第1类)的MF59佐剂血凝素(HA)疫苗接种了先前接种过0(H5N3)进化枝(初次接种)的受试者(A /鸭/新加坡/ 97)疫苗至少提前6年(在1999或2001年)。初免疫苗在单次加强疫苗接种后7天内迅速反应并产生了针对H5N1-越南菌株的高中和抗体滴度。此外,针对H5N1进化枝0、1和2病毒测定了显着的交叉中和效价。在当前的研究中,通过表面等离振子共振(SPR)的实时动力学分析,进一步评估了异源引发过程中MF59佐剂对不同疫苗组中体液多克隆免疫反应质量的影响。单次MF59-H5N1加强免疫后,异源初免-加强组的总抗H5N1 HA1多克隆血清抗体的结合显着高于接受两次MF59-H5N1疫苗接种的未初免个体的血清。 MF59-H5N3启动子组的多克隆血清针对H5N1-A /越南/ 1194/2004的HA1的抗原-抗体复合物解离速率(显着高于未佐剂的启动子组或未启动的个体的血清)接种了两种MF59-H5N1疫苗。此外,在针对HA1(而非HA2)的免疫血清的抗体解离解离速率与针对H5疫苗株和异源H5N1株的病毒中和效价之间观察到强反相关。这些发现支持使用水包油佐剂的大流行性流感疫苗来引发具有高亲和力BCR的长期记忆B细胞,该BCR能够对可能出现并适应人类传播的潜在变异大流行性病毒作出反应。

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