Prevalence of Helicobacter pylori vacA different genotypes in Isfahan, Iran
Background: It is believed that the Helicobacter pylori (H. pylori) vacA gene, as a major virulence determinant (One of the major virulence determinant, not major), may be a risk factor for the development of gastroduodenal diseases. The frequency of vacA genotypes varies in different human populati...
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doaj-4e15f996fd8c4363ad2be71732041ff82020-11-25T01:40:58ZengWolters Kluwer Medknow PublicationsAdvanced Biomedical Research2277-91752277-91752014-01-0131484810.4103/2277-9175.125761Prevalence of Helicobacter pylori vacA different genotypes in Isfahan, IranS Asghar HavaeiParviz MohajeriReza KhasheiRasoul SalehiHamid TavakoliBackground: It is believed that the Helicobacter pylori (H. pylori) vacA gene, as a major virulence determinant (One of the major virulence determinant, not major), may be a risk factor for the development of gastroduodenal diseases. The frequency of vacA genotypes varies in different human populations. This study evaluated the prevalence of vacA alleles/genotypes among dyspeptic patients in Isfahan. Materials and Methods: One-hundred H. pylori-positive adult patients were examined in this study. After culture of gastric biopsies and DNA extraction from individual H. pylori isolates, the (all H. pylori strains harbor vacA alleles, please replace "presence" with "genotypes") of the vacA s and m alleles were determined using polymerase chain reaction (PCR). Results: There were four vacA mosaicisms, including 28 for s1a/m1 (28%), 23 for s1b/m1 (23%), 26 for s1a/m2 (26%) and 23 for s1b/m2 (23%). The s2 allele was not found. The predominant vacA genotype in patients with non-ulcer dyspepsia and duodenal ulcer was s1a/m2, whereas in patients with adenocarcinoma was s1a/m1. Conclusion: The results showed there was no significant correlation between different genotypes of the vacA and the clinical outcomes and appears to vacA genotypes were not useful determinants for gastrointestinal diseases in our area.http://www.advbiores.net/article.asp?issn=2277-9175;year=2014;volume=3;issue=1;spage=48;epage=48;aulast=HavaeiAdenocarsinomagastroduodenal diseasesHelicobacter pyloriIranPeptic ulcerevacA gene |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
S Asghar Havaei Parviz Mohajeri Reza Khashei Rasoul Salehi Hamid Tavakoli |
spellingShingle |
S Asghar Havaei Parviz Mohajeri Reza Khashei Rasoul Salehi Hamid Tavakoli Prevalence of Helicobacter pylori vacA different genotypes in Isfahan, Iran Advanced Biomedical Research Adenocarsinoma gastroduodenal diseases Helicobacter pylori Iran Peptic ulcere vacA gene |
author_facet |
S Asghar Havaei Parviz Mohajeri Reza Khashei Rasoul Salehi Hamid Tavakoli |
author_sort |
S Asghar Havaei |
title |
Prevalence of Helicobacter pylori vacA different genotypes in Isfahan, Iran |
title_short |
Prevalence of Helicobacter pylori vacA different genotypes in Isfahan, Iran |
title_full |
Prevalence of Helicobacter pylori vacA different genotypes in Isfahan, Iran |
title_fullStr |
Prevalence of Helicobacter pylori vacA different genotypes in Isfahan, Iran |
title_full_unstemmed |
Prevalence of Helicobacter pylori vacA different genotypes in Isfahan, Iran |
title_sort |
prevalence of helicobacter pylori vaca different genotypes in isfahan, iran |
publisher |
Wolters Kluwer Medknow Publications |
series |
Advanced Biomedical Research |
issn |
2277-9175 2277-9175 |
publishDate |
2014-01-01 |
description |
Background: It is believed that the Helicobacter pylori (H. pylori) vacA gene, as a major virulence determinant (One of the major virulence determinant, not major), may be a risk factor for the development of gastroduodenal diseases. The frequency of vacA genotypes varies in different human populations. This study evaluated the prevalence of vacA alleles/genotypes among dyspeptic patients in Isfahan.
Materials and Methods: One-hundred H. pylori-positive adult patients were examined in this study. After culture of gastric biopsies and DNA extraction from individual H. pylori isolates, the (all H. pylori strains harbor vacA alleles, please replace "presence" with "genotypes") of the vacA s and m alleles were determined using polymerase chain reaction (PCR).
Results: There were four vacA mosaicisms, including 28 for s1a/m1 (28%), 23 for s1b/m1 (23%), 26 for s1a/m2 (26%) and 23 for s1b/m2 (23%). The s2 allele was not found. The predominant vacA genotype in patients with non-ulcer dyspepsia and duodenal ulcer was s1a/m2, whereas in patients with adenocarcinoma was s1a/m1.
Conclusion: The results showed there was no significant correlation between different genotypes of the vacA and the clinical outcomes and appears to vacA genotypes were not useful determinants for gastrointestinal diseases in our area. |
topic |
Adenocarsinoma gastroduodenal diseases Helicobacter pylori Iran Peptic ulcere vacA gene |
url |
http://www.advbiores.net/article.asp?issn=2277-9175;year=2014;volume=3;issue=1;spage=48;epage=48;aulast=Havaei |
work_keys_str_mv |
AT sasgharhavaei prevalenceofhelicobacterpylorivacadifferentgenotypesinisfahaniran AT parvizmohajeri prevalenceofhelicobacterpylorivacadifferentgenotypesinisfahaniran AT rezakhashei prevalenceofhelicobacterpylorivacadifferentgenotypesinisfahaniran AT rasoulsalehi prevalenceofhelicobacterpylorivacadifferentgenotypesinisfahaniran AT hamidtavakoli prevalenceofhelicobacterpylorivacadifferentgenotypesinisfahaniran |
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