Host repair polymorphisms and H. pylori genes in gastric disease outcomes: Who are the guardian and villains?

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS

ACS Applied Bio Materials Pub Date : 2024-10-09 DOI:10.1016/j.gene.2024.148977

Morgana Maria de Oliveira Barboza , Reginaldo Ferreira da Costa , João Paulo Por Deus Gomes , Rommel Mário Rodríguez Burbano , Paulo Goberlânio de Barros Silva , Silvia Helena Barem Rabenhorst

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Abstract

Gastric cancer (GC) is the fourth-leading cause of cancer-related mortality. The intestinal subtype of GC comes after the cascade of Correa, presenting H. pylori infection as the major etiological factor. One of the main mechanisms proposed for the progression from a more benign gastric lesion to cancer is DNA damage caused by chronic inflammation. Polymorphisms in DNA repair genes can lead to an imbalance of host DNA damage and repair, contributing to the development of GC. From there, we evaluated the risk of polymorphisms in DNA repair system genes in progressive gastric diseases and their association with the H. pylori genotype. This study included 504 patients from two public hospitals in Brazil’s north and northeast regions. The samples were classified into active and inactive gastritis, metaplasia, and GC. Polymorphisms in the DNA repair genes MLH1-93G > A, APE1 2197 T > G, XRCC1 28,152 G > A, MGMT 533 A > G, and XRCC3 18,067C > T were investigated by RFLP-PCR and H. pylori genotype by PCR. Statistical analyses were conducted using EPINFO 7.0., SNPSTAT, and CART software. The XRCC1 (GA) polymorphic allele stood out because it was associated with a lower risk of more severe gastric disease progression. Haplotypes of XRCC1 (GA) associated with some genotypes of MGMT, XRCC3, MLH1, and APE1 also showed protection against the progression of gastric diseases. XRCC3 (CT) showed a decreased risk of gastric disease progression in women, while a risk 1.3x to GC was observed in the MLH1 (A) polymorphic allele. The interaction between H. pylori genes and the host showed that the H. pylori cagE gene was the most important virulence factor associated with a worse clinical outcome, even overlapping with the XRCC1 polymorphism, where the MLH1 polymorphism response varied according to vacA alleles. Our results show the relevance of XRCC1 G > A for genome integrity, sex influence, and interaction between H. pylori virulence factors and XRCC1 and MLH1 genotypes for gastric lesion outcomes in Brazilian populations.

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胃病结局中的宿主修复多态性和幽门螺杆菌基因：谁是守护者，谁是恶棍？

胃癌（GC）是导致癌症相关死亡的第四大原因。肠道亚型胃癌出现在科雷亚级联之后，幽门螺杆菌感染是主要的致病因素。从良性胃病变发展为癌症的主要机制之一是慢性炎症造成的 DNA 损伤。DNA 修复基因的多态性可导致宿主 DNA 损伤和修复的失衡，从而导致胃癌的发生。由此，我们评估了DNA修复系统基因多态性在进展性胃病中的风险及其与幽门螺杆菌基因型的关联。这项研究包括来自巴西北部和东北部地区两家公立医院的 504 名患者。样本分为活动性和非活动性胃炎、化生期和 GC。通过 RFLP-PCR 调查了 DNA 修复基因 MLH1-93G > A、APE1 2197 T > G、XRCC1 28,152 G > A、MGMT 533 A > G 和 XRCC3 18,067C > T 的多态性，并通过 PCR 调查了幽门螺杆菌的基因型。统计分析使用 EPINFO 7.0、SNPSTAT 和 CART 软件进行。XRCC1（GA）多态等位基因与较低的严重胃病进展风险相关，因此脱颖而出。与 MGMT、XRCC3、MLH1 和 APE1 的某些基因型相关的 XRCC1 (GA) 单倍型也显示出对胃病进展的保护作用。XRCC3（CT）显示女性胃病恶化的风险降低，而 MLH1（A）多态等位基因的风险是 GC 的 1.3 倍。幽门螺杆菌基因与宿主之间的相互作用表明，幽门螺杆菌 cagE 基因是与较差临床结局相关的最重要毒力因子，甚至与 XRCC1 多态性重叠，而 MLH1 多态性的反应随 vacA 等位基因的不同而不同。我们的研究结果表明，在巴西人群中，XRCC1 G > A 与基因组完整性、性别影响以及幽门螺杆菌毒力因子与 XRCC1 和 MLH1 基因型之间的交互作用对胃部病变结果具有相关性。

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来源期刊

ACS Applied Bio Materials Chemistry-Chemistry (all)

CiteScore

9.40

自引率

2.10%

发文量

464