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幽门螺杆菌新型共毒力标志物 homB 的等位基因多样性和系统发育分析。

Allelic diversity and phylogeny of homB, a novel co-virulence marker of Helicobacter pylori.

机构信息

Departamento de Doenças Infecciosas, Instituto Nacional Saúde Dr Ricardo Jorge, Av. Padre Cruz, 1649-016 Lisboa, Portugal.

出版信息

BMC Microbiol. 2009 Dec 2;9:248. doi: 10.1186/1471-2180-9-248.

Abstract

BACKGROUND

The homB gene is a Helicobacter pylori disease-marker candidate, strongly associated with peptic ulcer disease, while homA, its paralogue gene with 90% sequence identity, is correlated with non-ulcer dyspepsia. The HomB encoded outer membrane protein was shown to contribute to the proinflammatory properties of H. pylori and also to be involved in bacterial adherence.This study investigated the distribution of homB and homA genes in 455 H. pylori strains from East Asian and Western countries, and carried out sequence comparison and phylogenetic analyses.

RESULTS

Both homB and homA genes were heterogeneously distributed worldwide, with a marked difference between East Asian and Western strains.Analysis of homB and homA sequences revealed diversity regarding the number of copies and their genomic localization, with East Asian and Western strains presenting different genotypes. Moreover, homB and homA sequence analysis suggests regulation by phase variation. It also indicates possible recombination events, leading to gene duplication or homB/homA conversion which may as well be implicated in the regulation of these genes. Phylogenetic reconstruction of homB and homA revealed clustering according to the geographic origin of strains. Allelic diversity in the middle region of the genes was observed for both homB and homA, although there was no correlation between any allele and disease. For each gene, a dominant worldwide allele was detected, suggesting that homB/homA allelic variants were independent of the geographical origin of the strain. Moreover, all alleles were demonstrated to be expressed in vivo.

CONCLUSION

Overall, these results suggest that homB and homA genes are good candidates to be part of the pool of H. pylori OMPs implicated in host-bacteria interface and also contributing to the generation of antigenic variability, and thus involved in H. pylori persistence.

摘要

背景

homB 基因是幽门螺杆菌疾病标记候选基因,与消化性溃疡病强烈相关,而其 90%序列相同的同源基因 homA 与非溃疡性消化不良相关。研究表明,HomB 编码的外膜蛋白有助于幽门螺杆菌的促炎特性,也参与细菌黏附。本研究调查了来自东亚和西方国家的 455 株幽门螺杆菌中 homB 和 homA 基因的分布情况,并进行了序列比较和系统发育分析。

结果

homB 和 homA 基因在全球范围内呈异质性分布,东亚和西方菌株之间存在显著差异。homB 和 homA 序列分析显示,其拷贝数和基因组定位存在多样性,东亚和西方菌株具有不同的基因型。此外,homB 和 homA 序列分析表明存在相位变异的调控。还表明可能存在重组事件,导致基因重复或 homB/homA 转换,这也可能涉及这些基因的调控。homB 和 homA 的系统发育重建显示,根据菌株的地理来源聚类。homB 和 homA 的基因中部观察到等位基因多样性,但任何等位基因与疾病均无相关性。对于每个基因,都检测到一个占主导地位的全球等位基因,这表明 homB/homA 等位基因变体与菌株的地理起源无关。此外,所有等位基因均在体内表达。

结论

总体而言,这些结果表明 homB 和 homA 基因是宿主-细菌界面中涉及的幽门螺杆菌 OMPs 的候选基因,也有助于产生抗原变异性,从而参与幽门螺杆菌的持续存在。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/376a/2795765/f9ebb2042888/1471-2180-9-248-1.jpg

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