首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >From the Cover: Metastability of Helicobacter pylori bab adhesin genes and dynamics in Lewis b antigen binding
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From the Cover: Metastability of Helicobacter pylori bab adhesin genes and dynamics in Lewis b antigen binding

机译:从封面:幽门螺杆菌婴儿粘附素基因的亚稳定性和Lewis b抗原结合的动力学

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摘要

Heterogeneity among Helicobacter pylori strains in gastric epithelial adherence is postulated to contribute to pathogen fitness in the physiologically diverse human population. H. pylori adherence to ABO and Lewis b (Leb) blood group antigens in the human stomach is mediated by the blood group antigen-binding adhesin BabA. Approximately 70% of Swedish and U.S. H. pylori clinical isolates exhibit Leb binding, but here we show that the babA gene is present in each of 10 Leb-nonbinding strains. Fluorescence microscopy identified occasional bacterial cells with a Leb-binding phenotype in populations of Leb-nonbinding strains. Thus, nonbinding seemed to be a metastable phenotype. To model metastable transition into the virulence-associated Leb-binding mode, Leb-binding clones were isolated from nonadherent strains by panning with Leb-magnetic beads and characterized. Strain 17875 has two babA genes, babA1 (silent) and babA2 (expressed). We found that a babA2-cam derivative of strain 17875 regained Leb binding by recombination of the formerly silent babA1 gene into the expressed and partially homologous babB locus. The chimeric BabB/A adhesin binds Leb with an affinity similar to that of wild-type BabA adhesin, but its expression level was lower and was subject to phase variation through slipped-strand mispairing. Equivalent results were obtained with strain NCTC11638. We propose that adhesin metastability and heterogeneity contributes to bacterial fitness and results in some clones having potential for periodic activation and deactivation of virulence appropriate for intensity of the host response to infection.
机译:幽门螺杆菌菌株在胃上皮粘附中的异质性被认为有助于病原体在不同生理人群中的适应性。幽门螺杆菌对人胃中ABO和Lewis b(Leb)血型抗原的粘附是由血型抗原结合粘附素BabA介导的。瑞典和美国幽门螺杆菌临床分离株中约有70%表现出Leb结合,但在这里我们表明babA基因存在于10种Leb非结合菌株中。荧光显微镜鉴定出在不结合Leb的菌株中偶尔出现具有Leb结合表型的细菌细胞。因此,非结合似乎是亚稳态的表型。为了模拟亚稳态过渡到毒力相关的Leb结合模式,通过用Leb磁珠淘选从非粘附菌株中分离出Leb结合克隆并进行了表征。菌株17875有两个babA基因,babA1(沉默)和babA2(表达)。我们发现,菌株17875的babA2-cam衍生物通过将以前沉默的babA1基因重组到表达的和部分同源的babB基因座中,重新获得了Leb结合。嵌合的BabB / A黏附素以与野生型BabA黏附素相似的亲和力结合Leb,但其表达水平较低,并由于滑链错配而发生相变。用菌株NCTC11638获得了等效的结果。我们提出,粘附素的亚稳态和异质性有助于细菌适应性,并导致某些克隆具有潜在的周期性激活和减毒能力,以适应宿主对感染的反应强度。

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