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重组感染因子群体中菌株结构的维持。

The maintenance of strain structure in populations of recombining infectious agents.

作者信息

Gupta S, Maiden M C, Feavers I M, Nee S, May R M, Anderson R M

机构信息

Wellcome Centre for the Epidemiology of Infectious Disease, Department of Zoology, University of Oxford, Oxford, UK.

出版信息

Nat Med. 1996 Apr;2(4):437-42. doi: 10.1038/nm0496-437.

Abstract

Using mathematical models that combine population genetic and epidemiological processes, we resolve the paradox that many important pathogens appear to persist as discrete strains despite the constant exchange of genetic material. We show that dominant polymorphic determinants (that is, those that elicit the most effective immune responses) will be organized into nonoverlapping combinations as a result of selection by the host immune system, thereby defining a set of discrete independently transmitted strains. By analysing 222 isolates of Neisseria meningitidis, we show that two highly polymorphic epitopes of the outer membrane protein PorA exist in nonoverlapping combinations as predicted by this general framework. The model indicates that dominant polymorphic determinants will be in linkage disequilibrium, despite frequent genetic exchange, even though they may be encoded by several unlinked genes. This suggests that the detection of nonrandom associations between epitope regions can be employed as a novel strategem for identifying dominant polymorphic antigens.

摘要

通过结合群体遗传学和流行病学过程的数学模型,我们解决了一个悖论:尽管遗传物质不断交换,但许多重要病原体似乎以离散菌株的形式持续存在。我们表明,由于宿主免疫系统的选择,显性多态性决定簇(即那些引发最有效免疫反应的决定簇)将被组织成不重叠的组合,从而定义了一组离散的独立传播菌株。通过分析222株脑膜炎奈瑟菌分离株,我们发现外膜蛋白PorA的两个高度多态性表位以该通用框架预测的不重叠组合存在。该模型表明,尽管频繁进行基因交换,但显性多态性决定簇仍将处于连锁不平衡状态,即使它们可能由几个不连锁的基因编码。这表明,检测表位区域之间的非随机关联可作为鉴定显性多态性抗原的一种新策略。

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