BACKGROUND: Long-term evaluation of gastric pathology after H. pylori infection is very important in order to reveal its clinical implications, since debate still exists on the gastric carcinogenesis provoked by H. pylori infection in animal models. AIM: Either to evaluate the long-term outcome of H. pylori infection or to determine how H. pylori could provoke gastric cancer in the mice model. METHODS: Four-week-old specific pathogen free C57BL/6 mice (n = 115) were infected with SS1, the mouse-adapted H. pylori strain. After 4, 8, 16, 24, 36, 50 and 80 weeks of bacterial infection, the H. pylori-infected mice were sacrificed. RESULTS: After 80 weeks of infection, almost all the H. pylori-infected mice developed hyperplastic gastritis, but did not show any evidence of gastric adenoma, dysplasia or carcinoma. PCNA positive cells were most abundant after 50 weeks and tended to decrease thereafter up to 80 weeks, whereas apoptosis began to be noted 8 weeks after H. pylori infection, showing 7-8 apoptotic cells/high power field, and tending to increase as time passed. Normally observed neutral mucin decreased during the experiment, showing the most marked decrease 50 weeks after H. pylori infection. In contrast, acidic mucin was noted from 50 weeks after infection. CONCLUSION: The SS1-infected mouse seems to be a suitable animal model for H. pylori-related research, and H. pylori itself does not induce gastric cancer in normal wild-type mouse model following long-term exposure, which could be explained by the balance that exists between cell proliferation and apoptosis.
BACKGROUND: Long-term evaluation of gastric pathology after H. pyloriinfection is very important in order to reveal its clinical implications, since debate still exists on the gastric carcinogenesis provoked by H. pyloriinfection in animal models. AIM: Either to evaluate the long-term outcome of H. pyloriinfection or to determine how H. pylori could provoke gastric cancer in the mice model. METHODS: Four-week-old specific pathogen free C57BL/6 mice (n = 115) were infected with SS1, the mouse-adapted H. pylori strain. After 4, 8, 16, 24, 36, 50 and 80 weeks of bacterial infection, the H. pylori-infectedmice were sacrificed. RESULTS: After 80 weeks of infection, almost all the H. pylori-infectedmice developed hyperplastic gastritis, but did not show any evidence of gastric adenoma, dysplasia or carcinoma. PCNA positive cells were most abundant after 50 weeks and tended to decrease thereafter up to 80 weeks, whereas apoptosis began to be noted 8 weeks after H. pyloriinfection, showing 7-8 apoptotic cells/high power field, and tending to increase as time passed. Normally observed neutral mucin decreased during the experiment, showing the most marked decrease 50 weeks after H. pyloriinfection. In contrast, acidic mucin was noted from 50 weeks after infection. CONCLUSION: The SS1-infectedmouse seems to be a suitable animal model for H. pylori-related research, and H. pylori itself does not induce gastric cancer in normal wild-type mouse model following long-term exposure, which could be explained by the balance that exists between cell proliferation and apoptosis.
Authors: Songhua Zhang; Dong Soo Lee; Rhiannon Morrissey; Jose R Aponte-Pieras; Arlin B Rogers; Steven F Moss Journal: Cancer Lett Date: 2014-09-11 Impact factor: 8.679
Authors: Y Gao; A Baccarelli; X O Shu; B-T Ji; K Yu; L Tarantini; G Yang; H-L Li; L Hou; N Rothman; W Zheng; Y-T Gao; W-H Chow Journal: Br J Cancer Date: 2011-12-15 Impact factor: 7.640
Authors: Ju Yup Lee; Nayoung Kim; Ryoung Hee Nam; Yoon Jeong Choi; Ji Hyung Seo; Hye Seung Lee; Jane C Oh; Dong Ho Lee Journal: J Cancer Prev Date: 2014-06