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Suppression of intestinal polyposis in Apc(delta 716) knockout mice by an additional mutation in the cytosolic phospholipase A(2) gene.胞质磷脂酶A2基因中的额外突变抑制Apc(δ716)基因敲除小鼠的肠道息肉形成
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HGF triggers activation of the COX-2 gene in rat gastric epithelial cells: action mediated through the ERK2 signaling pathway.肝细胞生长因子触发大鼠胃上皮细胞中COX-2基因的激活:通过ERK2信号通路介导的作用。
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大鼠肠上皮细胞中环氧合酶-2的转录后调控

Posttranscriptional regulation of cyclooxygenase-2 in rat intestinal epithelial cells.

作者信息

Zhang Z, Sheng H, Shao J, Beauchamp R D, DuBois R N

机构信息

Department of Medicine, Vanderbilt University Medical Center, Nashville, TN 37232, USA.

出版信息

Neoplasia. 2000 Nov-Dec;2(6):523-30. doi: 10.1038/sj.neo.7900117.

DOI:10.1038/sj.neo.7900117
PMID:11228545
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1508084/
Abstract

Modulation of cyclooxygenase-2 (COX-2) mRNA stability plays an important role in the regulation of its expression by oncogenic Ras. Here, we evaluate COX-2 mRNA stability in response to treatment with two known endogenous promoters of gastrointestinal cancer, the bile acid (chenodeoxycholate; CD) and ceramide. Treatment with CD and ceramide resulted in a 10-fold increase in the level of COX-2 protein and a four-fold lengthening of the half-life of COX-2 mRNA. COX-2 mRNA stability was assessed by Northern blot analysis and by evaluating the AU-rich element located in the COX-2 3'-UTR. A known inhibitor of mitogen-activated protein (MAP)/extracellular signal-regulated kinase (ERK) kinase (MEK), PD98059, reversed the effects of CD or ceramide to stabilize COX-2 mRNA. Overexpression of a dominant-negative ERK-1 or ERK-2 protein also led to destabilization of COX-2 mRNA. Treatment with a p38 MAPK inhibitor, PD169316, or transfection with a dominant-negative p38 MAPK construct reversed the effect of CD or ceramide to stabilize COX-2 mRNA. Expression of a dominant-negative c-Jun N-terminal kinase (JNK) had no effect on COX-2 mRNA stability in cells treated with CD or ceramide. We conclude that posttranscriptional mechanisms play an important role in the regulation of COX-2 expression during carcinogenesis.

摘要

环氧化酶-2(COX-2)信使核糖核酸(mRNA)稳定性的调节在致癌性Ras对其表达的调控中起着重要作用。在此,我们评估了COX-2 mRNA稳定性对两种已知的胃肠道癌内源性启动子——胆汁酸(鹅去氧胆酸盐;CD)和神经酰胺处理的反应。用CD和神经酰胺处理导致COX-2蛋白水平增加了10倍,COX-2 mRNA半衰期延长了4倍。通过Northern印迹分析以及评估位于COX-2 3'-非翻译区(UTR)的富含AU元件来评估COX-2 mRNA稳定性。一种已知的丝裂原活化蛋白(MAP)/细胞外信号调节激酶(ERK)激酶(MEK)抑制剂PD98059可逆转CD或神经酰胺对稳定COX-2 mRNA的作用。显性负性ERK-1或ERK-2蛋白的过表达也导致COX-2 mRNA不稳定。用p38 MAPK抑制剂PD169316处理或用显性负性p38 MAPK构建体转染可逆转CD或神经酰胺对稳定COX-2 mRNA的作用。显性负性c-Jun氨基末端激酶(JNK)的表达对用CD或神经酰胺处理的细胞中COX-2 mRNA稳定性没有影响。我们得出结论,转录后机制在致癌过程中COX-2表达的调控中起重要作用。