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局部高突变是脑膜炎奈瑟菌在持续性无症状带菌期间遗传变异性的主要驱动因素。

Localized Hypermutation is the Major Driver of Meningococcal Genetic Variability during Persistent Asymptomatic Carriage.

机构信息

Department of Genetics and Genome Biology, University of Leicester, Leicester, United Kingdom.

Department of Zoology, University of Oxford, Oxford, United Kingdom.

出版信息

mBio. 2020 Mar 24;11(2):e03068-19. doi: 10.1128/mBio.03068-19.

Abstract

Host persistence of bacteria is facilitated by mutational and recombinatorial processes that counteract loss of genetic variation during transmission and selection from evolving host responses. Genetic variation was investigated during persistent asymptomatic carriage of Interrogation of whole-genome sequences for paired isolates from 25 carriers showed that mutations were infrequent, while horizontal gene transfer occurred in 16% of carriers. Examination of multiple isolates per time point enabled separation of sporadic and transient allelic variation from directional variation. A comprehensive comparative analysis of directional allelic variation with hypermutation of simple sequence repeats and hyperrecombination of class 1 type IV pilus genes detected an average of seven events per carrier and 2:1 bias for changes due to localized hypermutation. Directional genetic variation was focused on the outer membrane with 69% of events occurring in genes encoding enzymatic modifiers of surface structures or outer membrane proteins. Multiple carriers exhibited directional and opposed switching of allelic variants of the surface-located Opa proteins that enables continuous expression of these adhesins alongside antigenic variation. A trend for switching from PilC1 to PilC2 expression was detected, indicating selection for specific alterations in the activities of the type IV pilus, whereas phase variation of restriction modification (RM) systems, as well as associated phasevarions, was infrequent. We conclude that asymptomatic meningococcal carriage on mucosal surfaces is facilitated by frequent localized hypermutation and horizontal gene transfer affecting genes encoding surface modifiers such that optimization of adhesive functions occurs alongside escape of immune responses by antigenic variation. Many bacterial pathogens coexist with host organisms, rarely causing disease while adapting to host responses. , a major cause of meningitis and septicemia, is a frequent persistent colonizer of asymptomatic teenagers/young adults. To assess how genetic variation contributes to host persistence, whole-genome sequencing and hypermutable sequence analyses were performed on multiple isolates obtained from students naturally colonized with meningococci. High frequencies of gene transfer were observed, occurring in 16% of carriers and affecting 51% of all nonhypermutable variable genes. Comparative analyses showed that hypermutable sequences were the major mechanism of variation, causing 2-fold more changes in gene function than other mechanisms. Genetic variation was focused on genes affecting the outer membrane, with directional changes in proteins responsible for bacterial adhesion to host surfaces. This comprehensive examination of genetic plasticity in individual hosts provides a significant new platform for rationale design of approaches to prevent the spread of this pathogen.

摘要

细菌在宿主体内的持续存在是由突变和重组过程促进的,这些过程可以防止在传播过程中遗传变异的损失,并对抗宿主反应的进化选择。我们在 25 名无症状带菌者的配对分离株的全基因组序列中进行了遗传变异的研究,结果表明突变很少发生,而水平基因转移发生在 16%的带菌者中。对每个时间点的多个分离株进行检查,能够将散在和短暂的等位基因变异与定向变异区分开来。对简单重复序列的超突变和 I 类 IV 型菌毛基因的超重组的定向等位基因变异的全面比较分析,检测到每个带菌者平均有 7 个事件,并且由于局部超突变导致的变化存在 2:1 的偏向性。定向遗传变异集中在外膜上,有 69%的事件发生在编码表面结构或外膜蛋白的酶修饰基因中。多个带菌者表现出表面定位的 Opa 蛋白的定向和相反的等位基因变异的切换,这使得这些黏附素能够与抗原变异一起连续表达。检测到从 PilC1 到 PilC2 表达的转换趋势,表明对 IV 型菌毛活性的特定改变的选择,而限制修饰(RM)系统的相变异和相关的相变异很少发生。我们的结论是,粘膜表面无症状脑膜炎奈瑟菌的携带是由频繁的局部超突变和水平基因转移引起的,这些突变和转移影响编码表面修饰物的基因,从而在通过抗原变异逃避免疫反应的同时优化黏附功能。许多细菌病原体与宿主生物共存,很少引起疾病,同时适应宿主反应。脑膜炎奈瑟菌是脑膜炎和败血症的主要原因,是无症状青少年/年轻人的常见持续性定植菌。为了评估遗传变异如何促进宿主的持续存在,我们对从自然定植脑膜炎奈瑟菌的学生中获得的多个分离株进行了全基因组测序和高突变序列分析。观察到高频率的基因转移,发生在 16%的带菌者中,影响了所有非高突变可变基因的 51%。比较分析表明,高突变序列是变异的主要机制,导致基因功能变化的频率是其他机制的两倍。遗传变异集中在影响外膜的基因上,负责细菌与宿主表面黏附的蛋白质发生定向变化。这项对个体宿主遗传可塑性的全面研究为预防这种病原体传播的合理方法提供了一个重要的新平台。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5dc3/7157529/acf19e8b5d81/mBio.03068-19-f0001.jpg

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