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首页> 外文期刊>Journal of Clinical Microbiology >Identification and Analysis of a NewvacA Genotype Variant of Helicobacter pylori in Different Patient Groups in Germany
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Identification and Analysis of a NewvacA Genotype Variant of Helicobacter pylori in Different Patient Groups in Germany

机译:德国不同患者群体中幽门螺杆菌NewvacA基因型变异体的鉴定和分析

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The vacuolating cytotoxin of Helicobacter pylori (VacA) is known to cause cell damage to mammalian cells and is suspected to give rise to gastric epithelial lesions that might lead to peptic ulcer disease. As shown recently, the gene encoding VacA exhibits genetic variation, with three different families of signal sequences (s1a, s1b, and s2) and two families of midregion sequences (m1 and m2). In order to investigate the relationship between the presence of specificvacA genotypes and peptic ulceration, the vacAgenotypes of 158 clinical isolates of H. pylori were determined. The study group consisted of 106 patients with duodenal ulceration; 52 patients with nonulcer dyspepsia (NUD) were used as controls. H. pylori of genotype s1 was isolated from 96% of the patients with ulcerations, whereas genotype s2 was only present in 4%, indicating a strong correlation between thevacA genotype and peptic ulceration (P < 0.001). In contrast, 31% of the patients from the NUD control group were infected with strains of vacA genotype s2. Particular midregion genotypes (m1 and m2) were not associated with clinical manifestations. The midregions from 18% of the isolates could not be classified by the proposed scheme. DNA sequencing revealed high homology between the untypeable midregions and that of genotype m1, with multiple base pair exchanges, some affecting the primer annealing site. Compared to those of m1 and m2 alleles, the divergent midregions from untypeable strains showed clustering, indicating the presence of a further subfamily of sequences in the midregion of vacA in German isolates, for which we propose the term “m1a.” A new specific primer that we designed for typing m1a isolates might be useful in other studies.
机译:幽门螺杆菌(VacA)的空泡细胞毒素已知会对哺乳动物细胞造成细胞损伤,并被怀疑会引起胃上皮损伤,从而可能导致消化性溃疡。如最近所示,编码VacA的基因表现出遗传变异,具有三个不同的信号序列家族(s1a,s1b和s2)和两个中间区域序列家族(m1和m2)。为研究158种 H临床分离株的 vacA 基因型与消化性溃疡之间的关系。确定了幽门螺旋杆菌。该研究组由106名十二指肠溃疡患者组成。 52例非溃疡性消化不良(NUD)患者用作对照。 H。从96%的溃疡患者中分离出了s1型幽门螺杆菌,而s2基因型仅占4%,表明 vacA 基因型与消化性溃疡( > P <0.001)。相反,NUD对照组中31%的患者感染了 vacA 基因型s2菌株。特定的中部区域基因型(m1和m2)与临床表现无关。提议的方案无法对来自18%分离株的中部地区进行分类。 DNA测序显示不可分的中间区域与基因型m1的中间区域具有高度同源性,具有多个碱基对交换,其中一些影响引物退火位点。与m1和m2等位基因相比,来自无法分型菌株的不同中部区域表现出聚类,表明在德国分离物中 vacA 的中部区域存在另一个亚家族序列,为此我们提出“ m1a。”我们设计用于键入m1a分离株的新的特异性引物可能在其他研究中有用。

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