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甲型流感的渐进式阶段性演变:来自简单模型的启示。

Influenza A gradual and epochal evolution: insights from simple models.

机构信息

UMR 7625 (UPMC, ENS, AgroParisTech, CNRS), Ecole Normale Supérieure, Unit of Eco-Evolutionary Mathematics, Paris, France.

出版信息

PLoS One. 2009 Oct 20;4(10):e7426. doi: 10.1371/journal.pone.0007426.

Abstract

The recurrence of influenza A epidemics has originally been explained by a "continuous antigenic drift" scenario. Recently, it has been shown that if genetic drift is gradual, the evolution of influenza A main antigen, the haemagglutinin, is punctuated. As a consequence, it has been suggested that influenza A dynamics at the population level should be approximated by a serial model. Here, simple models are used to test whether a serial model requires gradual antigenic drift within groups of strains with the same antigenic properties (antigenic clusters). We compare the effect of status based and history based frameworks and the influence of reduced susceptibility and infectivity assumptions on the transient dynamics of antigenic clusters. Our results reveal that the replacement of a resident antigenic cluster by a mutant cluster, as observed in data, is reproduced only by the status based model integrating the reduced infectivity assumption. This combination of assumptions is useful to overcome the otherwise extremely high model dimensionality of models incorporating many strains, but relies on a biological hypothesis not obviously satisfied. Our findings finally suggest the dynamical importance of gradual antigenic drift even in the presence of punctuated immune escape. A more regular renewal of susceptible pool than the one implemented in a serial model should be part of a minimal theory for influenza at the population level.

摘要

甲型流感疫情的反复出现最初可以用“连续抗原漂移”的情景来解释。最近,人们已经发现,如果遗传漂移是渐进的,那么甲型流感的主要抗原——血凝素的进化就是间断的。因此,有人提出,应该用一个连续模型来近似流感在人群水平上的动态。在这里,我们使用简单的模型来检验连续模型是否需要在具有相同抗原特性(抗原簇)的菌株群体中发生渐进的抗原漂移。我们比较了基于状态和基于历史的框架的影响,以及降低敏感性和感染性假设对抗原簇暂态动力学的影响。我们的结果表明,只有在整合了降低感染性假设的基于状态的模型中,才能重现数据中观察到的常驻抗原簇被突变簇所取代的现象。这种假设的组合有助于克服否则包含许多菌株的模型极高的模型维数,但依赖于一个并非明显满足的生物学假设。我们的研究结果最终表明,即使存在间断性免疫逃逸,渐进的抗原漂移在动力学上也是重要的。在人群水平上,流感的最小理论应该包括比连续模型中更有规律的易感人群更新。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/396e/2759541/d8db0ec95e30/pone.0007426.g001.jpg

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