COX-2减轻胃炎症和促进胃癌发生作用的体外证据。

K. Hahm, Ho Yeong Lim, S. Sohn, Hyuk Jae Kwon, K-Myung Lee, Jeong‐Sang Lee, Y. Surh, Young‐Bae Kim, H. Joo, Won-Seok Kim, Seung-Won Cho
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引用次数: 20

摘要

虽然胃腺癌是世界上最常见的恶性肿瘤之一,但对其发生发展的确切分子过程知之甚少。最近的研究表明,COX-2在胃肠道癌症的癌变中起重要作用,特别是在家族性腺瘤病息肉病小鼠模型中参与癌变。为了了解COX-2在胃癌发生和幽门螺杆菌相关性胃炎中的作用,我们通过免疫组织化学分析测量了170例人胃癌组织中COX-2的表达,并比较了COX-2在正常和癌粘膜配对组织中的表达。通过建立稳定的过表达COX-2的细胞系,获得了COX-2参与胃炎和胃癌发生的进一步证据。将COX-2亚克隆至pCB7哺乳动物表达载体后,转染COX-2 cDNA,获得了两个稳定的细胞系MKN-28-COX-2和MKN-45-COX-2。为了了解COX-2对胃炎的影响,我们对NF-kappaB(炎症相关转录因子)进行了电泳迁移性转移测定,并在幽门螺杆菌(1 × 10(6) CFU/mL)和中性粒细胞(10(2)个细胞/mL)刺激后,测量了模拟转染的MKN和MKN-COX-2细胞的丙二醛水平和化学荧光活性。在COX-2过表达的细胞中观察到NF-kappaB结合的明显衰减和自由基的产生。另一组实验,包括tgf - β处理的生长抑制、Matrigel侵袭实验和细胞凋亡实验。COX-2通过降低tgf - β RII的表达和增加细胞侵袭性,显示出摆脱tgf - β生长抑制的优势。综上所述,COX-2的表达似乎可以减轻萎缩性胃炎的程度,促进胃癌的发生。萎缩性胃炎是胃癌发生的初始事件。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
In vitro evidence of the role of COX-2 in attenuating gastric inflammation and promoting gastric carcinogenesis.
Although gastric adenocarcinoma is one of the most common malignancies in the world, little is known about its exact molecular processes in development and progression. Recent studies suggest that COX-2 is important in carcinogenesis of gastrointestinal cancers, and is especially involved in carcinogenesis in a mouse model of familial adenomatosis polyposis. To understand the role of COX-2 in gastric carcinogenesis and Helicobacter pylori-associated gastritis, we measured COX-2 expression in 170 human gastric carcinoma tissues byimmunohistochemical analysis and compared the expression of COX-2 in paired tissues obtained from normal-looking and cancer-bearing mucosa. Further evidence of the involvement of COX-2 in gastritis and gastric carcinogenesis was obtained by establishing stable cell lines overexpressing COX-2. After subcloning of COX-2 into pCB7 mammalian expression vector, two stable cell lines named MKN-28-COX-2 and MKN-45-COX-2 were generated by transfection of COX-2 cDNA. To understand the effect of COX-2 on gastritis, we performed an electrophoretic mobility shift assay of NF-kappaB (inflammation-associated transcription factor), and measured malondialdehyde levels and chemiluminescence activities in both mock-transfected MKN and MKN-COX-2 cells after stimulation of H. pylori (1 x 10(6) CFU/mL) and neutrophils (10(2) cells/mL). A marked attenuation of NF-kappaB bindings and generation of free radicals was observed in COX-2 overexpressed cells. Another set of experiments, including the growth inhibition by TGF-beta treatment, Matrigel invasion assay, and apoptosis assay, was done. COX-2 showed the advantage of the escape from the growth inhibition by TGF-beta through decreasing TGF-beta RII expression and increased cell invasiveness. In conclusion, COX-2 expression seems to be induced to attenuate the degree of atrophic gastritis, the initial event in gastric carcinogenesis, and promote gastric carcinogenesis.
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