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幽门螺杆菌临床分离株中vacA基因型与遗传多样性

vacA genotypes and genetic diversity in clinical isolates of Helicobacter pylori.

作者信息

Han S R, Schreiber H J, Bhakdi S, Loos M, Maeurer M J

机构信息

Department of Medical Microbiology, Johannes Gutenberg University, Mainz, Germany.

出版信息

Clin Diagn Lab Immunol. 1998 Mar;5(2):139-45. doi: 10.1128/CDLI.5.2.139-145.1998.

Abstract

Genetic diversity in Helicobacter pylori strains may affect the function and antigenicity of virulence factors associated with bacterial infection and, ultimately, disease outcome. In this study, DNA diversity of H. pylori isolates was examined by analysis of vacA genotypes and by restriction fragment length polymorphism (RFLP) analysis of H. pylori-associated genes (vacA, cagA,flaA, ureAB, and ureCD). Thirty-seven H. pylori isolates from 26 patients were successfully classified into distinct vacA allelic genotypes. The signal sequence allele sl (31 of 37) predominated over the s2 allele (6 of 37) and was significantly associated with the occurrence (past or present) of gastric ulcers. A novel midregion allele, designated as m3, has been identified in two H. pylori isolates which could not be typed with midregion allele m1- or m2-specific primers. Additionally, significant nucleotide diversity yielding different amino acid sequences was demonstrated by DNA sequencing of vacA fragments from clinical isolates of H. pylori. Furthermore, RFLP analysis of 45 H. pylori isolates (including 15 paired isolates) obtained from antrum and corpus biopsy specimens from 30 individual patients showed remarkably high interhost diversity (one patient, one H. pylori strain) and intrahost identity in gene sequences coding for VacA, CagA, flagellin, and urease. Only in a single patient was a minor genotypic variation at different anatomic sites within the stomach identified. These data warrant the detailed analysis of the effect of genetic diversity on the function and antigenicity of H. pylori-associated virulence factors.

摘要

幽门螺杆菌菌株的基因多样性可能会影响与细菌感染相关的毒力因子的功能和抗原性,并最终影响疾病的结局。在本研究中,通过分析vacA基因型以及对幽门螺杆菌相关基因(vacA、cagA、flaA、ureAB和ureCD)进行限制性片段长度多态性(RFLP)分析,检测了幽门螺杆菌分离株的DNA多样性。从26例患者中分离出的37株幽门螺杆菌被成功分类为不同的vacA等位基因型。信号序列等位基因s1(37株中的31株)比s2等位基因(37株中的6株)更占优势,并且与胃溃疡的发生(过去或现在)显著相关。在两株幽门螺杆菌分离株中鉴定出一种新的中间区域等位基因,命名为m3,这两株分离株无法用中间区域等位基因m1或m2特异性引物进行分型。此外,通过对幽门螺杆菌临床分离株的vacA片段进行DNA测序,证明了产生不同氨基酸序列的显著核苷酸多样性。此外,对从30例个体患者的胃窦和胃体活检标本中获得的45株幽门螺杆菌分离株(包括15对配对分离株)进行RFLP分析,结果显示在编码VacA、CagA、鞭毛蛋白和脲酶的基因序列中,宿主间多样性非常高(一个患者,一株幽门螺杆菌菌株),而宿主内具有同一性。仅在一名患者的胃内不同解剖部位发现了微小的基因型变异。这些数据有必要详细分析基因多样性对幽门螺杆菌相关毒力因子的功能和抗原性的影响。

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