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首页> 外文期刊>Canadian journal of microbiology >Microarray analysis of Streptococcus pneumoniae gene expression changes to human lung epithelial cells.
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Microarray analysis of Streptococcus pneumoniae gene expression changes to human lung epithelial cells.

机译:肺炎链球菌基因表达对人肺上皮细胞表达变化的微阵列分析。

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Streptococcus pneumoniae infection starts from the respiratory tract where interaction with host epithelial cells occurs. To gain more insights on pneumococcal pathogenesis, an oligonucleotide (oligo)-based microarray was used to investigate gene expression changes of one serotype 3 encapsulated pathogenic S. pneumoniae strain 82 and one unencapsulated avirulent S. pneumoniae strain R6 upon exposure to human lung epithelial cells (A549) for 1 and 3 h, respectively. We observed that genes associated with many functional categories were differentially regulated in strain 82, such as genes in pathogenesis, cell envelope, transcription, translation, transport, metabolism, and unknown functions. In contrast, few genes were changed in strain R6 except for genes in ribonucleotide biosynthesis and unknown functions. Quantitative real-time PCR analysis confirmed the microarray results for most of the genes tested. To further characterize functions of the selected genes, knockout mutants were constructed in strain R6. We demonstrated that 2 genetic loci, SP_2170 (AdcB, zinc ABC transporter) and SP_0157 (hypothetical protein), were involved in adherence to A549 cells. These data suggest that divergent gene expression changes occur in S. pneumoniae pathogenic and avirulent strains during interaction with human lung epithelial cells. Some of those genes are involved in pneumococcal pathogenesis.
机译:肺炎链球菌感染始于与宿主上皮细胞发生相互作用的呼吸道。为了获得更多关于肺炎球菌发病机理的见解,基于寡核苷酸(寡核苷酸)的微阵列被用于研究一种血清型3封装的致病性肺炎链球菌菌株82和一种未封装的无毒力肺炎链球菌菌株R6在暴露于人肺上皮细胞后的基因表达变化。 (A549)分别放置1和3小时。我们观察到与许多功能类别相关的基因在品系82中受到差异调节,例如发病机理,细胞包膜,转录,翻译,转运,代谢和未知功能中的基因。相反,除了核糖核苷酸生物合成的基因和未知功能外,菌株R6中几乎没有基因改变。实时定量PCR分析证实了大多数测试基因的微阵列结果。为了进一步表征所选基因的功能,在菌株R6中构建了敲除突变体。我们证明了2个遗传基因座SP_2170(AdcB,锌ABC转运蛋白)和SP_0157(假设蛋白)参与了对A549细胞的粘附。这些数据表明,在与人肺上皮细胞相互作用的过程中,肺炎链球菌的致病性和无毒力菌株发生了不同的基因表达变化。这些基因中的一些与肺炎球菌的发病机理有关。

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