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首页> 外文期刊>World Journal of Gastroenterology >Association of the myeloperoxidase (-468)G-A polymorphism with gastric inflammation and duodenal ulcer risk.
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Association of the myeloperoxidase (-468)G-A polymorphism with gastric inflammation and duodenal ulcer risk.

机译:髓过氧化物酶(-468)G-A多态性与胃炎症和十二指肠溃疡风险的关系。

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摘要

AIM: To elucidate the relations between the myeloperoxidase (-468)G-A polymorphism and the development of duodenal ulcer (DU), and to investigate the impacts of this host genetic polymorphism on the histopathological features of Helicobacter pylori (H pylori)-related gastritis. METHODS: In a case-control study of 115 consecutive DU patients and 182 controls, the myeloperoxidase (-468)G-A polymorphism was genotyped. Additionally, gastric mucosal changes were examined according to the updated Sydney System. RESULTS: The two study groups differed in the distributions of myeloperoxidase genotypes (P = 0.008). All six individuals carrying myeloperoxidase A/A genotypes were in the DU group. The carriage of myeloperoxidase allele A and H pylori infection were associated with an increased risk of DU with odds ratios (OR) of 2.3 and 5.8, respectively. The combined risk of the carriage of myeloperoxidase allele A and H pylori infection for DU was 8.7 (95% CI, 3.5-21.8). In the H pylori-infected individuals, allele A carriers displayed higher bacterial density scores (P = 0.04) in the antrum than did non-carriers. CONCLUSION: This work verifies for the first time the association of myeloperoxidase (-468)G-A polymorphism with antral H pylori density and DU disease. The mechanisms underlying this genetic polymorphism in developing DU disease merit further investigations.
机译:目的:阐明髓过氧化物酶(-468)G-A多态性与十二指肠溃疡(DU)的发展之间的关系,并研究该宿主基因多态性对幽门螺杆菌(H pylori)相关胃炎的组织病理学特征的影响。方法:在115例连续DU患者和182例对照的病例对照研究中,对髓过氧化物酶(-468)G-A多态性进行了基因分型。另外,根据更新的悉尼系统检查了胃粘膜变化。结果:两个研究组的髓过氧化物酶基因型分布不同(P = 0.008)。携带髓过氧化物酶A / A基因型的所有6个人均属于DU组。髓过氧化物酶等位基因A和H幽门螺杆菌感染的携带与DU风险增加相关,比值比(OR)分别为2.3和5.8。 DU携带髓过氧化物酶等位基因A和H幽门螺杆菌感染的总风险为8.7(95%CI,3.5-21.8)。在幽门螺杆菌感染的个体中,等位基因A携带者在胃窦比非携带者表现出更高的细菌密度得分(P = 0.04)。结论:这项工作首次验证了髓过氧化物酶(-468)G-A多态性与胃窦幽门螺杆菌密度和DU疾病的相关性。这种遗传多态性发展为DU疾病的潜在机制值得进一步研究。

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