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Hemagglutinin Sequence Conservation Guided Stem Immunogen Design from Influenza A H3 Subtype

机译:甲型H3流感病毒的血凝素序列保守性引导干免疫原设计

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Seasonal epidemics caused by influenza A (H1 and H3 subtypes) and B viruses are a major global health threat. The traditional, trivalent influenza vaccines have limited efficacy because of rapid antigenic evolution of the circulating viruses. This antigenic variability mediates viral escape from the host immune responses, necessitating annual vaccine updates. Influenza vaccines elicit a protective antibody response, primarily targeting the viral surface glycoprotein hemagglutinin (HA). However, the predominant humoral response is against the hypervariable head domain of HA, thereby restricting the breadth of protection. In contrast, the conserved, subdominant stem domain of HA is a potential “universal” vaccine candidate. We designed an HA stem-fragment immunogen from the 1968 pandemic H3N2 strain (A/Hong Kong/1/68) guided by a comprehensive H3 HA sequence conservation analysis. The biophysical properties of the designed immunogen were further improved by C-terminal fusion of a trimerization motif, “isoleucine-zipper”, or “foldon”. These immunogens elicited cross-reactive, antiviral antibodies and conferred partial protection against a lethal, homologous HK68 virus challenge in vivo . Furthermore, bacterial expression of these immunogens is economical and facilitates rapid scale-up.
机译:由甲型流感(H1和H3亚型)和乙型病毒引起的季节性流行病是主要的全球健康威胁。由于循环病毒的快速抗原进化,传统的三价流感疫苗的功效有限。这种抗原变异性介导病毒从宿主免疫反应中逃逸,需要每年更新疫苗。流感疫苗引起保护性抗体应答,主要针对病毒表面糖蛋白血凝素(HA)。然而,主要的体液反应是针对HA的高变头部结构域,从而限制了保护的广度。相反,HA的保守的,主要的茎结构域是潜在的“通用”疫苗候选物。在全面的H3 HA序列保守性分析的指导下,我们设计了1968年大流行H3N2菌株(A / Hong Kong / 1/68)的HA干片段免疫原。通过三聚体基序,“异亮氨酸拉链”或“ foldon”的C端融合进一步改善了设计免疫原的生物物理特性。这些免疫原在体内引起交叉反应的抗病毒抗体,并赋予了针对致命的同源HK68病毒攻击的部分保护。此外,这些免疫原的细菌表达是经济的,并有助于快速扩大规模。

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