Department of Pharmacology, Weill Medical College of Cornell University, New York, New York, United States of America.
PLoS One. 2010 Jul 6;5(7):e11451. doi: 10.1371/journal.pone.0011451.
Gastric cancer is the second leading cause of cancer death worldwide. Predisposing factors include achlorhydria, Helicobacter pylori infection, oxyntic atrophy and TFF2-expressing metaplasia. In parietal cells, apical potassium channels comprising the KCNQ1 alpha subunit and the KCNE2 beta subunit provide a K(+) efflux current to facilitate gastric acid secretion by the apical H(+)K(+)ATPase. Accordingly, genetic deletion of murine Kcnq1 or Kcne2 impairs gastric acid secretion. Other evidence has suggested a role for KCNE2 in human gastric cancer cell proliferation, independent of its role in gastric acidification. Here, we demonstrate that 1-year-old Kcne2(-/-) mice in a pathogen-free environment all exhibit a severe gastric preneoplastic phenotype comprising gastritis cystica profunda, 6-fold increased stomach mass, increased Ki67 and nuclear Cyclin D1 expression, and TFF2- and cytokeratin 7-expressing metaplasia. Some Kcne2(-/-) mice also exhibited pyloric polypoid adenomas extending into the duodenum, and neoplastic invasion of thin walled vessels in the sub-mucosa. Finally, analysis of human gastric cancer tissue indicated reduced parietal cell KCNE2 expression. Together with previous findings, the results suggest KCNE2 disruption as a possible risk factor for gastric neoplasia.
胃癌是全球癌症死亡的第二大主要原因。易患因素包括胃酸缺乏、幽门螺杆菌感染、胃窦萎缩和 TFF2 表达的化生。在壁细胞中,由 KCNQ1α亚基和 KCNE2β亚基组成的顶端钾通道提供 K+外流通路,以促进顶端 H+K+ATP 酶的胃酸分泌。因此,鼠类 Kcnq1 或 Kcne2 的基因缺失会损害胃酸分泌。其他证据表明,KCNE2 在人类胃癌细胞增殖中具有作用,这与其在胃酸酸化中的作用无关。在这里,我们证明在无病原体环境中,1 岁的 Kcne2(-/-) 小鼠均表现出严重的胃前瘤表型,包括囊状胃炎、胃质量增加 6 倍、Ki67 和核 Cyclin D1 表达增加以及 TFF2 和细胞角蛋白 7 表达的化生。一些 Kcne2(-/-) 小鼠还表现出幽门息肉状腺瘤延伸到十二指肠,以及黏膜下层薄壁血管的肿瘤性浸润。最后,对人胃癌组织的分析表明壁细胞 KCNE2 表达减少。结合以前的发现,结果表明 KCNE2 缺失可能是胃癌发生的一个危险因素。
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