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Genetic Analysis of Helicobacter pylori Strain Populations Colonizing the Stomach at Different Times Postinfection

机译:感染后不同时间在胃中定植的幽门螺杆菌菌株群体的遗传分析

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摘要

Genetic diversity of the human gastric pathogen Helicobacter pylori in an individual host has been observed; whether this diversity represents diversification of a founding strain or a mixed infection with distinct strain populations is not clear. To examine this issue, we analyzed multiple single-colony isolates from two to four separate stomach biopsies of eight adult and four pediatric patients from a high-incidence Mexican population. Eleven of the 12 patients contained isolates with identical random amplified polymorphic DNA, amplified fragment length polymorphism, and vacA allele molecular footprints, whereas a single adult patient had two distinct profiles. Comparative genomic hybridization using whole-genome microarrays (array CGH) revealed variation in 24 to 67 genes in isolates from patients with similar molecular footprints. The one patient with distinct profiles contained two strain populations differing at 113 gene loci, including the cag pathogenicity island virulence genes. The two strain populations in this single host had different spatial distributions in the stomach and exhibited very limited genetic exchange. The total genetic divergence and pairwise genetic divergence between isolates from adults and isolates from children were not statistically different. We also analyzed isolates obtained 15 and 90 days after experimental infection of humans and found no evidence of genetic divergence, indicating that transmission to a new host does not induce rapid genetic changes in the bacterial population in the human stomach. Our data suggest that humans are infected with a population of closely related strains that vary at a small number of gene loci, that this population of strains may already be present when an infection is acquired, and that even during superinfection genetic exchange among distinct strains is rare.
机译:已经观察到人胃病原体幽门螺杆菌在单个宿主中的遗传多样性。这种多样性是否代表建立菌株的多样化或具有不同菌株种群的混合感染尚不清楚。为了研究这个问题,我们分析了来自高发病率墨西哥人群的八名成人和四名儿科患者的两次至四个独立的胃活检样本中的多个单菌落。 12例患者中有11例包含具有相同随机扩增多态性DNA,扩增片段长度多态性和vacA等位基因分子足迹的分离株,而一名成年患者则具有两个不同的特征。使用全基因组微阵列(阵列CGH)进行的比较基因组杂交显示,具有相似分子足迹的患者分离物中的24至67个基因存在变异。一位具有不同特征的患者包含两个在113个基因位点不同的菌株种群,包括cag致病性岛毒力基因。该单一宿主中的两个菌株群体在胃中具有不同的空间分布,并且表现出非常有限的遗传交换。成人分离株和儿童分离株之间的总遗传差异和成对遗传差异在统计学上没有差异。我们还分析了人类实验性感染后15天和90天获得的分离株,没有发现遗传差异的证据,这表明向新宿主的传播不会在人胃中引起细菌种群的快速遗传变化。我们的数据表明,人类感染了一群密切相关的菌株,这些菌株在少数基因位点处变化,当获得感染后,该菌株群体可能已经存在,并且即使在超级感染过程中,不同菌株之间的遗传交换也是罕见。

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