1.Characterizing Helicobacter pylori cagA in Myanmar
Thein MYINT ; Muhammad MIFTAHUSSURUR ; Ratha korn VILAICHONE ; New NI ; Than Than AYE ; Phawinee SUBSOMWONG ; Tomohisa UCHIDA ; Varocha MAHACHAI ; Yoshio YAMAOKA
Gut and Liver 2018;12(1):51-57
BACKGROUND/AIMS: Differences in the Helicobacter pylori infection rate are not sufficient to clarify the dissimilarity of gastric cancer incidence between Myanmar and its neighboring countries. To better understand this trend, the H. pylori virulence gene cagA was characterized in Myanmar. METHODS: Glutamate-proline-isoleucine-tyrosine-alanine (EPIYA) patterns and CagA multimerization (CM) motifs of cagA genotypes were examined by performing polymerase chain reactions and DNA sequencing. RESULTS: Of 69 tested H. pylori strains, cagA-positive patients had significantly more severe histological scores in their antrum than cagA-negative patients. Sequence analysis revealed that 94.1% of strains had Western-type cagA containing an EPIYA motif (92.6%) or EPIYT motif (6.4%). The intestinal metaplasia scores in the antral of patients infected with the ABC and ABCC types of cagA were significantly higher than those of patients with AB-type cagA. Interestingly, in patients infected with H. pylori, 46.3% of strains with three EPIYA motifs contained two identical Western-typical CM motifs, and these patients showed significantly higher antrum inflammation scores than patients infected with two identical nontypical-CM motif strains (p=0.02). CONCLUSIONS: In Myanmarese strains, Western-type cagA was predominant. The presence of CM motifs and the proportion of multiple EPIYA-C segments might partially explain the intermediate gastric cancer risk found in Myanmar.
Genotype
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Helicobacter pylori
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Helicobacter
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Humans
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Incidence
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Inflammation
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Metaplasia
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Myanmar
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Polymerase Chain Reaction
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Sequence Analysis
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Sequence Analysis, DNA
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Stomach Neoplasms
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Virulence
2.Utilization of an Automated Latex Agglutination Turbidity Assay for Assessing Gastric Mucosal Alteration during Helicobacter pylori Infection
Ayush KHANGAI ; Junko AKADA ; Batsaikhan SARUULJAVKHLAN ; Boldbaatar GANTUYA ; Dashdorj AZZAYA ; Khasag OYUNTSETSEG ; Duger DAVAADORJ ; Tomohisa UCHIDA ; Takashi MATSUMOTO ; Yoshio YAMAOKA
Gut and Liver 2024;18(1):60-69
Background/Aims:
A latex agglutination turbidity (LA) assay to test for serum antibodies has been approved in Japan and Korea for mass screening of Helicobacter pylori infection. In this study, we evaluated the LA assay for diagnosing H. pylori infection and predicting gastric mucosal changes in a Mongolian population.
Methods:
In total, 484 individuals were classified into H. pylori-positive (n=356) and H. pylorinegative (n=128) groups, as determined by histology and H. pylori culture.
Results:
The best cutoff, sensitivity, and specificity values for the LA assay were 18.35 U/mL, 74.2%, and 65.6%, respectively. The LA values in the atrophic gastritis group were statistically higher than those in the other groups (healthy, chronic gastritis, intestinal metaplasia, and gastric cancer, p<0.0001). The cutoff value to distinguish the atrophic gastritis group from the other four groups was 32.0 U/mL, and its area under the curve was 0.673, which was the highest among the E-plate, pepsinogen (PG) I, PG II, and PG I/II ratio tests in our data. The odds ratios for atrophic gastritis determined by the LA assay and PG I test in multiple logistic regression were 2.5 and 1.9, respectively, which were significantly higher than for the other tests.
Conclusions
The LA assay can determine the risk of atrophic gastritis, which in turn is a considerable risk factor for gastric cancer. We propose using this assay in combination with the PG I/II ratio to avoid missing gastric cancer patients who have a low LA value (less than 32.0 U/mL).