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在印度人群中,完整的dupA(dupA1)而非dupA1簇与十二指肠溃疡的关联。

Association of Intact dupA (dupA1) rather than dupA1 cluster with duodenal ulcer in Indian population.

作者信息

Alam Jawed, Ghosh Prachetash, Ganguly Mou, Sarkar Avijit, De Ronita, Mukhopadhyay Asish K

机构信息

Division of Bacteriology, National Institute of Cholera and Enteric Diseases, P 33, CIT Road, Scheme, XM Beliaghata.

出版信息

Gut Pathog. 2015 Mar 28;7:9. doi: 10.1186/s13099-015-0056-2. eCollection 2015.

Abstract

BACKGROUND

The duodenal ulcer promoting gene (dupA) and dupA cluster in Helicobacter pylori have been described as a risk factor for duodenal ulcer development in some populations. Polymorphic gene dupA can be divided into two groups, intact dupA1 (long or short type based on the presence or absence of 615-bp extra sequences at the 5' region) having complete reading frame and other truncated dupA2 having frame-shift mutation. This study was aimed to elucidate the role of dupA of H. pylori and their clusters in the disease manifestation of Indian population.

METHODS

A total of 170 H. pylori strains were screened for the presence of dupA, dupA alleles and dupA cluster by PCR and sequencing. Pro-inflammatory cytokine (IL-8) with different dupA variant H. pylori stimulated gastric epithelial cells (AGS cells) was measured by ELISA.

RESULTS

A total of 50 strains (29.4%) were positive for dupA among the tested 170 strains. The prevalence of dupA1 in duodenal ulcer (DU) and non-ulcer dyspepsia (NUD) populations was found to be 25.5% (25/98) and 11.1% (8/72), respectively and 16.4% (28/170) of the tested strains had dupA1, cagA and vacAs1m1 positive. The distribution of long and short type dupA1 has not been significantly associated with the disease outcome. The dupA cluster analysis showed that 10.2% (10/98) and 8.3% (6/72) strains were positive among DU and NUD, respectively. IL-8 production was significantly higher in dupA1(+) , cagA (+), vacA (+) (902.5 ± 79.01 pg/mL) than dupA2 (+) , cagA (+) , vacA (+) (536.0 ± 100.4 pg/mL, P = 0.008) and dupA (-), cagA (+), vacA (+) (549.7 ± 104.1 pg/mL, P = 0.009). Phylogenetic analysis of dupA indicated that the Indian H. pylori strains clustered with East Asian strains but distinct from Western strains. This is the first known genetic element of Indian H. pylori that is genetically closer to the East Asian strains but differed from the Western strains.

CONCLUSIONS

The intact dupA1 was significantly associated with DU than NUD (P = 0.029) but the dupA1 cluster has no role in the disease manifestation at India (P = 0.79). Thus, dupA1 can be considered as a biomarker for DU patients in India.

摘要

背景

幽门螺杆菌中的十二指肠溃疡促进基因(dupA)及其基因簇已被描述为某些人群十二指肠溃疡发生的危险因素。多态性基因dupA可分为两组,具有完整阅读框的完整dupA1(根据5'区域是否存在615 bp额外序列分为长型或短型)和其他具有移码突变的截短型dupA2。本研究旨在阐明幽门螺杆菌dupA及其基因簇在印度人群疾病表现中的作用。

方法

通过PCR和测序对总共170株幽门螺杆菌菌株进行dupA、dupA等位基因和dupA基因簇检测。用ELISA法检测不同dupA变异型幽门螺杆菌刺激胃上皮细胞(AGS细胞)后促炎细胞因子(IL-8)的产生。

结果

在检测的170株菌株中,共有50株(29.4%)dupA呈阳性。发现dupA1在十二指肠溃疡(DU)和非溃疡性消化不良(NUD)人群中的患病率分别为25.5%(25/98)和11.1%(8/72),且16.4%(28/170)的检测菌株dupA1、cagA和vacAs1m1呈阳性。长型和短型dupA1的分布与疾病结局无显著相关性。dupA基因簇分析显示,DU和NUD中分别有10.2%(10/98)和8.3%(6/72)的菌株呈阳性。dupA1(+)、cagA(+)、vacA(+)组的IL-8产生量(902.5±79.01 pg/mL)显著高于dupA2(+)、cagA(+)、vacA(+)组(536.0±100.4 pg/mL,P = 0.008)和dupA(-)、cagA(+)、vacA(+)组(549.7±104.1 pg/mL,P = 0.009)。dupA的系统发育分析表明,印度幽门螺杆菌菌株与东亚菌株聚类,但与西方菌株不同。这是印度幽门螺杆菌第一个已知的遗传元件,在基因上更接近东亚菌株,但与西方菌株不同。

结论

完整的dupA1与DU的相关性显著高于NUD(P = 0.029),但dupA1基因簇在印度的疾病表现中无作用(P = 0.79)。因此,dupA1可被视为印度DU患者的生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5739/4379697/f84f1e806499/13099_2015_56_Fig1_HTML.jpg

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