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本文引用的文献

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Population genomic datasets describing the post-vaccine evolutionary epidemiology of Streptococcus pneumoniae.描述肺炎链球菌疫苗接种后进化流行病学的人群基因组数据集。
Sci Data. 2015 Oct 27;2:150058. doi: 10.1038/sdata.2015.58. eCollection 2015.
2
Effect of Serotype on Pneumococcal Competition in a Mouse Colonization Model.血清型对小鼠定植模型中肺炎球菌竞争的影响。
mBio. 2015 Sep 15;6(5):e00902-15. doi: 10.1128/mBio.00902-15.
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Novel R tools for analysis of genome-wide population genetic data with emphasis on clonality.用于分析全基因组群体遗传数据(重点为克隆性)的新型R工具。
Front Genet. 2015 Jun 10;6:208. doi: 10.3389/fgene.2015.00208. eCollection 2015.
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FAST: FAST Analysis of Sequences Toolbox.FAST:序列分析工具箱
Front Genet. 2015 May 19;6:172. doi: 10.3389/fgene.2015.00172. eCollection 2015.
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Selective and genetic constraints on pneumococcal serotype switching.肺炎球菌血清型转换的选择性和遗传限制
PLoS Genet. 2015 Mar 31;11(3):e1005095. doi: 10.1371/journal.pgen.1005095. eCollection 2015 Mar.
6
Conserved surface accessible nucleoside ABC transporter component SP0845 is essential for pneumococcal virulence and confers protection in vivo.保守的表面可及核苷ABC转运蛋白组分SP0845对肺炎球菌毒力至关重要,并在体内提供保护。
PLoS One. 2015 Feb 17;10(2):e0118154. doi: 10.1371/journal.pone.0118154. eCollection 2015.
7
Rapid phylogenetic analysis of large samples of recombinant bacterial whole genome sequences using Gubbins.使用Gubbins对重组细菌全基因组序列的大量样本进行快速系统发育分析。
Nucleic Acids Res. 2015 Feb 18;43(3):e15. doi: 10.1093/nar/gku1196. Epub 2014 Nov 20.
8
Diversification of bacterial genome content through distinct mechanisms over different timescales.细菌基因组内容通过不同时间尺度上的不同机制实现多样化。
Nat Commun. 2014 Nov 19;5:5471. doi: 10.1038/ncomms6471.
9
Variable recombination dynamics during the emergence, transmission and 'disarming' of a multidrug-resistant pneumococcal clone.在一种多药耐药性肺炎球菌克隆的出现、传播和“解除武装”过程中,可变重组的动态变化。
BMC Biol. 2014 Jun 23;12:49. doi: 10.1186/1741-7007-12-49.
10
Evidence for soft selective sweeps in the evolution of pneumococcal multidrug resistance and vaccine escape.肺炎球菌多重耐药性和疫苗逃逸进化中软选择性清除的证据。
Genome Biol Evol. 2014 Jun 10;6(7):1589-602. doi: 10.1093/gbe/evu120.

通过全基因组范围的免疫学筛选鉴定出的肺炎球菌抗原的多样进化模式。

Diverse evolutionary patterns of pneumococcal antigens identified by pangenome-wide immunological screening.

作者信息

Croucher Nicholas J, Campo Joseph J, Le Timothy Q, Liang Xiaowu, Bentley Stephen D, Hanage William P, Lipsitch Marc

机构信息

Department of Infectious Disease Epidemiology, Imperial College London, London W2 1PG, United Kingdom;

Antigen Discovery Inc., Irvine, CA 92618.

出版信息

Proc Natl Acad Sci U S A. 2017 Jan 17;114(3):E357-E366. doi: 10.1073/pnas.1613937114. Epub 2017 Jan 4.

DOI:10.1073/pnas.1613937114
PMID:28053228
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5255586/
Abstract

Characterizing the immune response to pneumococcal proteins is critical in understanding this bacterium's epidemiology and vaccinology. Probing a custom-designed proteome microarray with sera from 35 healthy US adults revealed a continuous distribution of IgG affinities for 2,190 potential antigens from the species-wide pangenome. Reproducibly elevated IgG binding was elicited by 208 "antibody binding targets" (ABTs), which included 109 variants of the diverse pneumococcal surface proteins A and C (PspA and PspC) and zinc metalloprotease A and B (ZmpA and ZmpB) proteins. Functional analysis found ABTs were enriched in motifs for secretion and cell surface association, with extensive representation of cell wall synthesis machinery, adhesins, transporter solute-binding proteins, and degradative enzymes. ABTs were associated with stronger evidence for evolving under positive selection, although this varied between functional categories, as did rates of diversification through recombination. Particularly rapid variation was observed at some immunogenic accessory loci, including a phage protein and a phase-variable glycosyltransferase ubiquitous among the diverse set of genomic islands encoding the serine-rich PsrP glycoprotein. Nevertheless, many antigens were conserved in the core genome, and strains' antigenic profiles were generally stable. No strong evidence was found for any epistasis between antigens driving population dynamics, or redundancy between functionally similar accessory ABTs, or age stratification of antigen profiles. These results highlight the paradox of why substantial variation is observed in only a subset of epitopes. This result may indicate only some interactions between immunoglobulins and ABTs clear pneumococcal colonization or that acquired immunity to pneumococci is an accumulation of individually weak responses to ABTs evolving under different levels of functional constraint.

摘要

了解肺炎球菌蛋白质的免疫反应对于理解这种细菌的流行病学和疫苗学至关重要。用35名美国健康成年人的血清检测定制设计的蛋白质组微阵列,发现针对全物种泛基因组中2190种潜在抗原的IgG亲和力呈连续分布。208个“抗体结合靶点”(ABT)可重复性地引发IgG结合升高,其中包括多种肺炎球菌表面蛋白A和C(PspA和PspC)以及锌金属蛋白酶A和B(ZmpA和ZmpB)蛋白的109个变体。功能分析发现,ABT富含分泌和细胞表面结合基序,细胞壁合成机制、黏附素、转运溶质结合蛋白和降解酶广泛存在。ABT与在正选择下进化的更强证据相关,尽管这在功能类别之间有所不同,通过重组的多样化速率也是如此。在一些免疫原性辅助基因座观察到特别快速的变异,包括一种噬菌体蛋白和一种在编码富含丝氨酸的PsrP糖蛋白的不同基因组岛中普遍存在的相变糖基转移酶。然而,许多抗原在核心基因组中是保守的,菌株的抗原谱总体上是稳定的。没有发现驱动种群动态的抗原之间存在上位性、功能相似的辅助ABT之间存在冗余或抗原谱存在年龄分层的有力证据。这些结果凸显了为什么仅在一部分表位中观察到大量变异这一矛盾。这一结果可能表明,只有免疫球蛋白与ABT之间的某些相互作用才能清除肺炎球菌定植,或者对肺炎球菌的获得性免疫是对在不同功能限制水平下进化的ABT的个体微弱反应的积累。