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对群体水平的主要组织相容性复合体(MHC)多样性进行实验操作,可控制小家鼠病原体毒力的进化。

Experimental manipulation of population-level MHC diversity controls pathogen virulence evolution in Mus musculus.

作者信息

Cornwall D H, Kubinak J L, Zachary E, Stark D L, Seipel D, Potts W K

机构信息

Department of Biology, University of Utah, Salt Lake City, UT, USA.

University of South Carolina School of Medicine, Columbia, SC, USA.

出版信息

J Evol Biol. 2018 Feb;31(2):314-322. doi: 10.1111/jeb.13225. Epub 2018 Jan 12.

Abstract

The virulence levels attained by serial passage of pathogens through similar host genotypes are much higher than observed in natural systems; however, it is unknown what keeps natural virulence levels below these empirically demonstrated maximum levels. One hypothesis suggests that host diversity impedes pathogen virulence, because adaptation to one host genotype carries trade-offs in the ability to replicate and cause disease in other host genotypes. To test this hypothesis, with the simplest level of population diversity within the loci of the major histocompatibility complex (MHC), we serially passaged Friend virus complex (FVC) through two rounds, in hosts with either the same MHC genotypes (pure passage) or hosts with different MHC genotypes (alternated passage). Alternated passages showed a significant overall reduction in viral titre (31%) and virulence (54%) when compared to pure passages. Furthermore, a resistant host genotype initially dominated any effects due to MHC diversity; however, when FVC was allowed to adapt to the resistant host genotype, predicted MHC effects emerged; that is, alternated lines show reduced virulence. These data indicate serial exposure to diverse MHC genotypes is an impediment to pathogen adaptation, suggesting genetic variation at MHC loci is important for limiting virulence in a rapidly evolving pathogen and supports negative frequency-dependent selection as a force maintaining MHC diversity in host populations.

摘要

病原体通过相似宿主基因型进行连续传代所达到的毒力水平,远高于在自然系统中观察到的水平;然而,尚不清楚是什么因素使得自然毒力水平低于这些通过实验证明的最高水平。一种假说认为,宿主多样性会阻碍病原体的毒力,因为适应一种宿主基因型会在复制能力以及在其他宿主基因型中致病能力方面产生权衡。为了验证这一假说,我们利用主要组织相容性复合体(MHC)位点内最简单的种群多样性水平,让弗瑞德病毒复合体(FVC)在具有相同MHC基因型的宿主(纯传代)或具有不同MHC基因型的宿主(交替传代)中连续传代两轮。与纯传代相比,交替传代表现出病毒滴度显著总体降低(31%)以及毒力显著降低(54%)。此外,一种抗性宿主基因型最初主导了因MHC多样性产生的任何效应;然而,当FVC被允许适应抗性宿主基因型时,预测的MHC效应出现了;也就是说,交替传代的品系表现出毒力降低。这些数据表明,连续暴露于多样的MHC基因型会阻碍病原体的适应,这表明MHC位点的遗传变异对于限制快速进化病原体的毒力很重要,并支持负频率依赖选择作为维持宿主种群中MHC多样性的一种力量发挥作用。

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