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Construction, characterization, and immunization of nanoparticles that display a diverse array of influenza HA trimers

机译:纳米颗粒的构建,表征和免疫,显示多种流感HA三聚体阵列

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Current influenza vaccines do not elicit broadly protective immune responses against multiple strains. New strategies to focus the humoral immune response to conserved regions on influenza antigens are therefore required for recognition by broadly neutralizing antibodies. It has been suggested that B-cells with receptors that recognize conserved epitopes would be preferentially stimulated through avidity effects by mosaic particles presenting multiple forms of a variable antigen. We adapted SpyCatcher-based platforms, AP205 virus-like particles (VLPs) and mi3 nanoparticles (NPs), to covalently co-display SpyTagged hemagglutinin (HA) trimers from group 1 and group 2 influenza A strains. Here we show successful homotypic and heterotypic conjugation of up to 8 different HA trimers to both VLPs and NPs. We characterized the HA-VLPs and HA-NPs by cryo-electron tomography to derive the average number of conjugated HAs and their separation distances on particles, and compared immunizations of mosaic and homotypic particles in wild-type mice. Both types of HA particles elicited strong antibody responses, but the mosaic particles did not consistently elicit broader immune responses than mixtures of homotypic particles. We conclude that covalent attachment of HAs from currently-circulating influenza strains represents a viable alternative to current annual influenza vaccine strategies, but in the absence of further modifications, is unlikely to represent a method for making a universal influenza vaccine.
机译:目前的流感疫苗不会引发针对多种菌株的广泛保护性免疫应答。因此,需要通过宽度中和抗体来识别对流感抗原的保守区域进行体液免疫应答的新策略。已经提出,具有识别保守表位的受体的B细胞优先通过呈现多种形式的可变抗原的马赛克颗粒来刺激可亲和力的效果。我们适应了基于Spycatcher的平台,AP205病毒样颗粒(VLP)和Mi 3纳米颗粒(NPS),共价共价共同地与第1组和第2组流感菌株的血清血凝素(HA)三聚体。在这里,我们将多达8种不同的HA三种分子与VLP和NPS显示成功的同型和异相缀合。通过冷冻电子断层扫描来表征HA-VLP和HA-NPS,以导出颗粒上的共轭的平均数量及其分离距离,并在野生型小鼠中比较马赛克和均型颗粒的免疫。两种类型的HA颗粒引发了强烈的抗体反应,但是马赛克颗粒并未始终产生比均型颗粒的混合物的更广泛的免疫应答。我们得出结论,来自目前循环的流感菌株的共价附着代表了目前年度流感疫苗策略的可行替代品,但在没有进一步修改的情况下,不太可能代表一种制作普遍流感疫苗的方法。

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