Hahm Ki Baik, Song Young Joon, Oh Tae Young, Lee Jeong Sang, Surh Young-Joon, Kim Young Bae, Yoo Byung Moo, Kim Jin Hong, Han Sang Uk, Nahm Ki Taik, Kim Myung-Wook, Kim Dae Yong, Cho Sung Won
Chemoprevention Agent Development Research Group, Division of Cancer Prevention, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA.
J Biochem Mol Biol. 2003 Jan 31;36(1):82-94. doi: 10.5483/bmbrep.2003.36.1.082.
Although debates still exist whether Helicobacter pylori infection is really class I carcinogen or not, H. pylori has been known to provoke precancerous lesions like gastric adenoma and chronic atrophic gastritis with intestinal metaplasia as well as gastric cancer. Chronic persistent, uncontrolled gastric inflammations are possible basis for ensuing gastric carcinogenesis and H. pylori infection increased COX-2 expressions, which might be the one of the mechanisms leading to gastric cancer. To know the implication of long-term treatment of antiinflammatory drugs, rebamipide or nimesulide, on H. pylori-associated gastric carcinogenesis, we infected C57BL/6 mice with H. pylori, especially after MNU administration to promote carcinogenesis and the effects of the long-term administration of rebamipide or nimesulide were evaluated. C57BL/6 mice were sacrificed 50 weeks after H. pylori infection. Colonization rates of H. pylori, degree of gastric inflammation and other pathological changes including atrophic gastritis and metaplasia, serum levels and mRNA transcripts of various mouse cytokines and chemokines, and NF-kappaB binding activities, and finally the presence of gastric adenocarcinoma were compared between H. pylori infected group (HP), and H. pylori infected group administered with long-term rebamipide containing pellet diets (HPR) or nimesulide mixed pellets (HPN). Gastric mucosal expressions of ICAM-1, HCAM, MMP, and transcriptional regulations of NF-kappaB binding were all significantly decreased in HPR group than in HP group. Multi-probe RNase protection assay showed the significantly decreased mRNA levels of apoptosis related genes and various cytokines genes like IFN-gamma, RANTES, TNF-alpha, TNFR p75, IL-1beta in HPR group. In the experiment designed to provoke gastric cancer through MNU treatment with H. pylori infection, the incidence of gastric carcinoma was not changed between HP and HPR group, but significantly decreased in HPN group, suggesting the chemoprevention of H. pylori-associated gastric carcinogenesis by COX-2 inhibition. Long-term administration of antiinflammatory drugs should be considered in the treatment of H. pylori since they showed the molecular and biologic advantages with possible chemopreventive effect against H. pylori-associated gastric carcinogenesis. If the final concrete proof showing the causal relationship between H. pylori infection and gastric carcinogenesis could be obtained, that will shed new light on chemoprevention of gastric cancer, that is, that gastric cancer could be prevented through either the eradication of H. pylori or lessening the inflammation provoked by H. pylori infection in high risk group.
尽管关于幽门螺杆菌感染是否真的是I类致癌物仍存在争议,但已知幽门螺杆菌会引发癌前病变,如胃腺瘤、伴有肠化生的慢性萎缩性胃炎以及胃癌。慢性持续性、未得到控制的胃部炎症可能是随后胃癌发生的基础,而幽门螺杆菌感染会增加COX - 2的表达,这可能是导致胃癌的机制之一。为了了解抗炎药物瑞巴派特或尼美舒利的长期治疗对幽门螺杆菌相关胃癌发生的影响,我们用幽门螺杆菌感染C57BL/6小鼠,尤其是在给予MNU以促进致癌作用之后,并评估了瑞巴派特或尼美舒利长期给药的效果。幽门螺杆菌感染50周后处死C57BL/6小鼠。比较了幽门螺杆菌感染组(HP)、长期给予含瑞巴派特颗粒饲料的幽门螺杆菌感染组(HPR)和含尼美舒利混合颗粒的幽门螺杆菌感染组(HPN)之间的幽门螺杆菌定植率、胃部炎症程度以及包括萎缩性胃炎和化生在内的其他病理变化、各种小鼠细胞因子和趋化因子的血清水平和mRNA转录本、NF-κB结合活性,以及最终胃腺癌的存在情况。与HP组相比,HPR组中ICAM - 1、HCAM、MMP的胃黏膜表达以及NF-κB结合的转录调控均显著降低。多探针核糖核酸酶保护分析显示,HPR组中凋亡相关基因以及各种细胞因子基因如IFN-γ、RANTES、TNF-α、TNFR p75、IL-1β的mRNA水平显著降低。在通过MNU治疗并感染幽门螺杆菌来诱发胃癌的实验中,HP组和HPR组之间胃癌的发生率没有变化,但HPN组显著降低,这表明通过抑制COX - 2可对幽门螺杆菌相关胃癌发生起到化学预防作用。在幽门螺杆菌的治疗中应考虑长期使用抗炎药物,因为它们显示出分子和生物学优势,可能对幽门螺杆菌相关胃癌发生具有化学预防作用。如果能够获得显示幽门螺杆菌感染与胃癌发生之间因果关系的最终确凿证据,那将为胃癌的化学预防带来新的启示,即通过根除幽门螺杆菌或减轻高危人群中幽门螺杆菌感染引发的炎症来预防胃癌。
Zotero 插件