Premium
Cancer development based on chronic active gastritis and resulting gastric atrophy as assessed by serum levels of pepsinogen and Helicobacter pylori antibody titer
Author(s) -
Yoshida Takeichi,
Kato Jun,
Inoue Izumi,
Yoshimura Noriko,
Deguchi Hisanobu,
Mukoubayashi Chizu,
Oka Masashi,
Watanabe Mika,
Enomoto Shotaro,
Niwa Toru,
Maekita Takao,
Iguchi Mikitaka,
Tamai Hideyuki,
Utsunomiya Hirotoshi,
Yamamichi Nobutake,
Fujishiro Mitsuhiro,
Iwane Masataka,
Takeshita Tatsuya,
Ushijima Toshikazu,
Ichinose Masao
Publication year - 2013
Publication title -
international journal of cancer
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.475
H-Index - 234
eISSN - 1097-0215
pISSN - 0020-7136
DOI - 10.1002/ijc.28470
Subject(s) - helicobacter pylori , gastroenterology , medicine , cancer , chronic gastritis , gastritis , atrophic gastritis , hazard ratio , pepsin , asymptomatic , stomach cancer , titer , antibody , immunology , confidence interval , biology , biochemistry , enzyme
Our study investigated the relationship between gastric cancer development and activity of Helicobacter pylori ‐associated chronic gastritis or the resulting chronic atrophic gastritis (CAG). A cohort of 4,655 healthy asymptomatic subjects, in whom serum pepsinogen (PG) and H. pylori antibody titer had been measured to assess the activity and stage of H. pylori ‐associated chronic gastritis, was followed for up to 16 years, and cancer development was investigated. In subjects with a serologically diagnosed healthy stomach ( H. pylori ‐negative/CAG‐negative), cancer incidence rate was low, at 16/100,000 person‐years. With the establishment of H. pylori infection and progression of chronic gastritis, significant stepwise cancer risk elevations were seen from CAG‐free subjects ( H. pylori ‐positive/CAG‐negative) [hazard ratio (HR) = 8.9, 95% confidence interval (CI) = 2.7–54.7] to subjects with CAG ( H. pylori ‐positive/CAG‐positive) (HR = 17.7, 95% CI = 5.4–108.6) and finally to subjects with metaplastic gastritis ( H. pylori ‐negative/CAG‐positive) (HR = 69.7, 95% CI = 13.6–502.9). In H. pylori ‐infected CAG‐free subjects, significantly elevated cancer risk was observed in the subgroup with active inflammation‐based high PG II level or potent immune response‐based high H. pylori antibody titer; the former was associated with a particularly high risk of diffuse‐type cancer, and both subgroups showed high cancer incidence rates of around 250/100,000 person‐years, comparable to that in subjects with CAG. No such risk elevation was observed in H. pylori ‐infected subjects with CAG. These results clearly indicate that gastric cancer develops mainly from the gastritis‐atrophy‐metaplasia‐cancer sequence and partly from active inflammation‐based direct carcinogenesis, and that serum levels of PG and H. pylori antibody titer provide indices of cancer development in H. pylori ‐infected subjects.