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首页> 外文期刊>Philosophical Transactions of the Royal Society of London, Series B. Biological Sciences >Masking of antigenic epitopes by antibodies shapes the humoral immune response to influenza
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Masking of antigenic epitopes by antibodies shapes the humoral immune response to influenza

机译:抗体对抗原表位的掩盖塑造了针对流感的体液免疫反应

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The immune responses to influenza, a virus that exhibits strain variation, show complex dynamics where prior immunity shapes the response to the subsequent infecting strains. Original antigenic sin (OAS) describes the observation that antibodies to the first encountered influenza strain, specifically antibodies to the epitopes on the head of influenza's main surface glycoprotein, haemagglutinin (HA), dominate following infection with new drifted strains. OAS suggests that responses to the original strain are preferentially boosted. Recent studies also show limited boosting of the antibodies to conserved epitopes on the stem of HA, which are attractive targets for a 'universal vaccine'. We develop multi-epitope models to explore how pre-existing immunity modulates the immune response to new strains following immunization. Our models suggest that the masking of antigenic epitopes by antibodies may play an important role in describing the complex dynamics of OAS and limited boosting of antibodies to the stem of HA. Analysis of recently published data confirms model predictions for how pre-existing antibodies to an epitope on HA decrease the magnitude of boosting of the antibody response to this epitope following immunization. We explore strategies for boosting of antibodies to conserved epitopes and generating broadly protective immunity to multiple strains.
机译:对流感病毒(表现出菌株变异的病毒)的免疫反应显示出复杂的动态,其中先前的免疫力决定了对随后感染菌株的反应。原始抗原罪案(OAS)描述了以下观察结果:首先感染流感病毒株的抗体,特别是针对流感主要表面糖蛋白血凝素(HA)头部抗原决定簇的抗体,在新的漂移菌株感染后占主导地位。 OAS建议优先提高对原始菌株的反应。最近的研究还显示,针对HA茎上保守表位的抗体有限增强,这些表位是“通用疫苗”的有吸引力的靶标。我们开发多表位模型,以探索预先存在的免疫如何调节免疫后新菌株的免疫反应。我们的模型表明,抗体对抗原表位的掩盖可能在描述OAS的复杂动力学和抗体对HA茎的有限增强中起重要作用。对最近发表的数据的分析证实了模型预测,即在免疫后,HA上针对表位的预先存在的抗体如何降低增强对该表位的抗体应答的幅度。我们探索了增强针对保守表位的抗体并针对多种菌株产生广泛保护性免疫的策略。

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