[The association between Helicobacter pylori virulence factor genotypes and gastroduodenal diseases in children].

J J Ying, X L Shu, G Long, M Z Jiang
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Abstract

Objective: To investigate the association between Helicobacter pylori (Hp) virulence factor genotypes and the degree and activity of gastric mucosa pathological changes in pediatric gastroduodenal diseases. Methods: This retrospective cohort study was conducted from May 2020 to October 2020. The frozen strains of Hp, which were cultured with the gastric mucosa of 68 children with gastroscopy confirmed gastroduodenal diseases who visited the children's hospital of Zhejiang University School of Medicine from April 2012 to December 2014, were resuscitated. After extracting DNA from these Hp strains, PCR amplification and agarose gel electrophoresis were performed to determine the detection rate of cytotoxin-associated protein A (cagA),vacuolating cytotoxin A (vacA)(s1a、s1b/s2,m1/m2), outer inflammatory protein A (oipA),blood group antigen binding adhesin (babA),duodenal ulcer promoting protein A (dupA) genes; oipA genes were sequenced to determine the gene status. The patients were divided into different groups according to the findings of gastroscopy and gastric mucosa pathology. The detection rates of various virulence factor genotypes among different groups were compared using χ2 tests or Fisher's exact tests. Results: The 68 Hp strains all completed genetic testing. According to the diagnostic findings of gastroscopy, the 68 cases were divided into 47 cases of superficial gastritis and 21 cases of peptic ulcer. Regarding the pathological changes of gastric mucosa, 8 cases were mild, and 60 cases were moderate and severe according to the degree of inflammation; 61 cases were active and 7 cases inactive according to the activity of inflammation. The overall detection rates of cagA, vacA, vacA s1/m2, functional oipA, babA2, and dupA virulence factor genes were 100% (68/68), 100% (68/68), 94% (64/68), 99% (67/68), 82% (56/68), and 71% (48/68), respectively. In the superficial gastritis group, their detection rates were 100% (47/47), 100% (47/47), 96% (45/47), 98% (46/47), 81% (38/47), and 70% (33/47), respectively; in the peptic ulcer group, their detection rates were 100% (21/21), 100% (21/21), 90% (19/21), 100% (21/21), 86% (18/21), and 71% (15/21), respectively. There was no statistically significant difference between the two groups (all P>0.05). In the mild gastric mucosa inflammation group, the detection rates of the above six genotypes were 8/8, 8/8, 8/8, 7/8, 7/8, and 5/8, respectively; and in the moderate to severe inflammation groups, the detection rates were 100% (60/60), 100% (60/60), 93% (56/60), 100% (60/60), 82% (49/60), and 72% (43/60), respectively, with no statistically significant difference between the two groups (all P>0.05). In the active inflammation group, the detection rate of six genotypes were 100% (61/61), 100% (61/61), 93% (57/61), 98% (60/61), 82% (50/61), and 72% (44/61), respectively; and in the inactive inflammation group, they were 7/7, 7/7, 7/7, 7/7, 6/7, and 4/7, respectively. Again, there was no statistically significant difference between the two groups (all P>0.05). There was no statistically significant difference in the detection rate of combinations of 4 or 5 virulence factor genes among the different groups (all P>0.05). Conclusions: CagA, vacA, vacA s1/m2, functional oipA, babA2, and dupA genes are not associated with superficial gastritis and peptic ulcer in children, or with the degree and activity of gastric mucosa pathological inflammation. Different gene combinations of cagA, vacA, oipA, babA2, and dupA have no significant effects on predicting the clinical outcome of Hp infection in children.

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[幽门螺杆菌毒力因子基因型与儿童胃十二指肠疾病的关系]。
目的:探讨幽门螺杆菌(Hp)毒力因子基因型与小儿胃十二指肠疾病胃黏膜病变程度和活动性的关系。方法:回顾性队列研究于2020年5月至2020年10月进行。对2012年4月至2014年12月在浙江大学医学院儿童医院就诊的胃镜确诊胃十二指肠疾病的68例患儿的胃黏膜进行冷冻培养的Hp菌株进行复苏。提取Hp菌株DNA后,采用PCR扩增和琼脂糖凝胶电泳检测细胞毒素相关蛋白A (cagA)、空泡细胞毒素A (vacA)(s1a、s1b/s2、m1/m2)、外炎蛋白A (oipA)、血型抗原结合黏附素(babA)、十二指肠溃疡促进蛋白A (dupA)基因的检出率;对oipA基因进行测序以确定基因状态。根据胃镜检查和胃黏膜病理结果将患者分为不同的组。采用χ2检验或Fisher精确检验比较不同组间不同毒力因子基因型的检出率。结果:68株Hp均完成基因检测。根据胃镜检查结果,将68例患者分为浅表性胃炎47例,消化性溃疡21例。胃黏膜病理改变按炎症程度分为轻度8例,中、重度60例;根据炎症活动性,活动性61例,非活动性7例。cagA、vacA、vacA s1/m2、功能性oipA、babA2和dupA毒力因子基因的总检出率分别为100%(68/68)、100%(68/68)、94%(64/68)、99%(67/68)、82%(56/68)和71%(48/68)。浅表性胃炎组检出率分别为100%(47/47)、100%(47/47)、96%(45/47)、98%(46/47)、81%(38/47)、70% (33/47);消化性溃疡组检出率分别为100%(21/21)、100%(21/21)、90%(19/21)、100%(21/21)、86%(18/21)、71%(15/21)。两组间差异无统计学意义(均P>0.05)。在轻度胃黏膜炎症组,上述6种基因型的检出率分别为8/8、8/8、8/8、7/8、7/8、5/8;中重度炎症组的检出率分别为100%(60/60)、100%(60/60)、93%(56/60)、100%(60/60)、82%(49/60)、72%(43/60),两组比较差异均无统计学意义(P>0.05)。活动性炎症组6种基因型检出率分别为100%(61/61)、100%(61/61)、93%(57/61)、98%(60/61)、82%(50/61)、72% (44/61);非活性炎症组分别为7/7、7/7、7/7、7/7、6/7、4/7。两组间差异无统计学意义(均P>0.05)。4、5个毒力因子基因组合检出率各组间差异均无统计学意义(P>0.05)。结论:CagA、vacA、vacA s1/m2、功能性oipA、babA2、dupA基因与儿童浅表性胃炎和消化性溃疡无关,与胃黏膜病理性炎症的程度和活动性无关。cagA、vacA、oipA、babA2和dupA的不同基因组合对预测儿童Hp感染的临床结局无显著影响。
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