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Key importance of the Helicobacter pylori adherence factor blood group antigen binding adhesin during chronic gastric inflammation.
Cancer Res. 2001 Mar 01; 61(5):1903-9.CR

Abstract

Helicobacter pylori has been assigned as a class I carcinogen because of its relation to gastric adenocarcinoma. Chronic H. pylori infection may lead to severe gastritis, glandular atrophy (AT), and intestinal metaplasia (IM). Strains secreting the vacuolating toxin VacA and producing the cytotoxin-associated antigen CagA (type 1 strains), as well as the blood group antigen binding adhesin (BabA) targeting Lewis(b) antigens, have been associated previously with distal gastric adenocarcinoma (M. Gerhard et al., Proc. Natl. Acad. Sci. USA, 96: 12778-12783, 1999) and may therefore also be related to lesions preceding gastric cancer. Antral and corpus biopsies were collected from 451 patients; 151 were H. pylori positive, as determined by PCR. Gastric biopsies were histologically evaluated for activity of gastritis (G0-G3, granulocyte infiltration), chronicity of gastritis (L1-L3, lymphocyte infiltration), and the presence of IM and/or AT according to the Sydney classification. Simultaneously, the presence of bacterial genes encoding virulence and adherence factors (racAs1/s2, cagA, and babA2) was determined by PCR. The presence of cagA+ and vacAs1 (alone or combined) both correlated with activity and chronicity of gastritis (P < 0.05); however, the overall prevalence of these genes was 60 or 72%, respectively, and was thus relatively frequent. The babA2 gene, encoding the adhesin BabA, was detected in 38% of infected patients and was correlated with the activity of gastritis in antrum and corpus (P < 0.005). cagA+/vacAs1+ strains (suggesting the presence of type 1 strains) that were also babA2 positive were detected more frequently in patients with severe histological alterations (such as G3, IM, or AT) compared with subjects without these changes (P < 0.01). cagA+/vacAs1+ strains that were babA2 negative, however, lacked a significant correlation with severe histological changes, activity, or chronicity of gastritis in antrum and corpus. Adherence of H. pylori via BabA appears to be of importance for efficient delivery of VacA and CagA and may play a special role in the pathogenesis of severe histological changes.

Authors+Show Affiliations

Prinz C
Department of Medicine II and Gastroenterology, Bogenhausen Academic Teaching Hospital, Technical University, Munich, Germany. christian.prinz@lrz.tum.de
Schöniger M
No affiliation info available
Rad R
No affiliation info available
Becker I
No affiliation info available
Keiditsch E
No affiliation info available
Wagenpfeil S
No affiliation info available
Classen M
No affiliation info available
Rösch T
No affiliation info available
Schepp W
No affiliation info available
Gerhard M
No affiliation info available

MeSH

Adhesins, BacterialAdultAgedAged, 80 and overAntigens, BacterialBacterial ProteinsBacterial ToxinsBiopsyCarrier ProteinsChronic DiseaseFemaleGastritisGastritis, AtrophicGenotypeGranulocytesHelicobacter InfectionsHelicobacter pyloriHumansIntestinesLewis Blood Group AntigensLymphocytesMaleMetaplasiaMiddle AgedStomach

Pub Type(s)

Journal Article
Research Support, Non-U.S. Gov't

Language

eng

PubMed ID

11280745

Citation

Prinz, C, et al. "Key Importance of the Helicobacter Pylori Adherence Factor Blood Group Antigen Binding Adhesin During Chronic Gastric Inflammation." Cancer Research, vol. 61, no. 5, 2001, pp. 1903-9.
Prinz C, Schöniger M, Rad R, et al. Key importance of the Helicobacter pylori adherence factor blood group antigen binding adhesin during chronic gastric inflammation. Cancer Res. 2001;61(5):1903-9.
Prinz, C., Schöniger, M., Rad, R., Becker, I., Keiditsch, E., Wagenpfeil, S., Classen, M., Rösch, T., Schepp, W., & Gerhard, M. (2001). Key importance of the Helicobacter pylori adherence factor blood group antigen binding adhesin during chronic gastric inflammation. Cancer Research, 61(5), 1903-9.
Prinz C, et al. Key Importance of the Helicobacter Pylori Adherence Factor Blood Group Antigen Binding Adhesin During Chronic Gastric Inflammation. Cancer Res. 2001 Mar 1;61(5):1903-9. PubMed PMID: 11280745.
* Article titles in AMA citation format should be in sentence-case
TY - JOUR T1 - Key importance of the Helicobacter pylori adherence factor blood group antigen binding adhesin during chronic gastric inflammation. AU - Prinz,C, AU - Schöniger,M, AU - Rad,R, AU - Becker,I, AU - Keiditsch,E, AU - Wagenpfeil,S, AU - Classen,M, AU - Rösch,T, AU - Schepp,W, AU - Gerhard,M, PY - 2001/3/31/pubmed PY - 2001/4/21/medline PY - 2001/3/31/entrez SP - 1903 EP - 9 JF - Cancer research JO - Cancer Res VL - 61 IS - 5 N2 - Helicobacter pylori has been assigned as a class I carcinogen because of its relation to gastric adenocarcinoma. Chronic H. pylori infection may lead to severe gastritis, glandular atrophy (AT), and intestinal metaplasia (IM). Strains secreting the vacuolating toxin VacA and producing the cytotoxin-associated antigen CagA (type 1 strains), as well as the blood group antigen binding adhesin (BabA) targeting Lewis(b) antigens, have been associated previously with distal gastric adenocarcinoma (M. Gerhard et al., Proc. Natl. Acad. Sci. USA, 96: 12778-12783, 1999) and may therefore also be related to lesions preceding gastric cancer. Antral and corpus biopsies were collected from 451 patients; 151 were H. pylori positive, as determined by PCR. Gastric biopsies were histologically evaluated for activity of gastritis (G0-G3, granulocyte infiltration), chronicity of gastritis (L1-L3, lymphocyte infiltration), and the presence of IM and/or AT according to the Sydney classification. Simultaneously, the presence of bacterial genes encoding virulence and adherence factors (racAs1/s2, cagA, and babA2) was determined by PCR. The presence of cagA+ and vacAs1 (alone or combined) both correlated with activity and chronicity of gastritis (P < 0.05); however, the overall prevalence of these genes was 60 or 72%, respectively, and was thus relatively frequent. The babA2 gene, encoding the adhesin BabA, was detected in 38% of infected patients and was correlated with the activity of gastritis in antrum and corpus (P < 0.005). cagA+/vacAs1+ strains (suggesting the presence of type 1 strains) that were also babA2 positive were detected more frequently in patients with severe histological alterations (such as G3, IM, or AT) compared with subjects without these changes (P < 0.01). cagA+/vacAs1+ strains that were babA2 negative, however, lacked a significant correlation with severe histological changes, activity, or chronicity of gastritis in antrum and corpus. Adherence of H. pylori via BabA appears to be of importance for efficient delivery of VacA and CagA and may play a special role in the pathogenesis of severe histological changes. SN - 0008-5472 UR - https://www.unboundmedicine.com/medline/citation/11280745/Key_importance_of_the_Helicobacter_pylori_adherence_factor_blood_group_antigen_binding_adhesin_during_chronic_gastric_inflammation_ DB - PRIME DP - Unbound Medicine ER -
Grapherence [↓50]

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