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血栓素受体α的激活通过多种信号通路诱导A549人肺腺癌细胞中环氧化酶-2的表达。

Activation of thromboxane receptor alpha induces expression of cyclooxygenase-2 through multiple signaling pathways in A549 human lung adenocarcinoma cells.

作者信息

Wei Jingyan, Yan Weili, Li Xiuling, Chang Wen-Chang, Tai Hsin-Hsiung

机构信息

Department of Pharmaceutical Sciences, College of Pharmacy, University of Kentucky, Lexington, KY 40536-0082, United States.

出版信息

Biochem Pharmacol. 2007 Sep 1;74(5):787-800. doi: 10.1016/j.bcp.2007.06.008. Epub 2007 Jun 14.

DOI:10.1016/j.bcp.2007.06.008
PMID:17632087
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1995664/
Abstract

Human lung adenocarcinoma A549 cells stably transfected with TPalpha (A549-TPalpha) were used to study agonist I-BOP-induced expression of cyclooxygenase-2 (COX-2) and the related mechanisms of induced expression. I-BOP, a TP agonist, induced a time- and dose-dependent expression of COX-2 in A549-TPalpha cells. The signaling pathways of I-BOP-induced COX-2 expression were elucidated by using various inhibitors of the signaling molecules. The effects of these inhibitors were assessed at protein level, enzyme activity and promoter activity of COX-2. Within MAPK family, both ERK and p38 MAPK but not JNK/SAPK pathways were involved in the induction. Other pathways such as JAK/Stat3 pathway and beta-catenin/TCF/LEF pathway also participated in the induction. The activation of key signaling molecules, ERK, p38 MAPK, CREB and NF-kappaB, involved in the COX-2 transcription was further studied at the phosphorylation step. Activation of ERK and p38 MAPK appeared to be mediated primarily by transactivation of EGFR, whereas activation of CREB and NF-kappaB was mediated by PKA, PKC and ERK. The role of CREB and NF-kappaB in I-BOP-induced COX-2 expression was further explored at the promoter level. Studies on promoter fragments and mutation of responsive motifs indicated that CRE and NF-kappaB sites are critical for the COX-2 induction. Distal NF-kappaB site is essential for the basal induction of the COX-2 transcription, whereas CRE and proximal NF-kappaB sites are important for the induced transcription. These results indicate that I-BOP-induced COX-2 expression through multiple signaling pathways.

摘要

使用稳定转染TPα的人肺腺癌A549细胞(A549-TPα)来研究激动剂I-BOP诱导的环氧合酶-2(COX-2)表达及诱导表达的相关机制。I-BOP是一种TP激动剂,可在A549-TPα细胞中诱导COX-2呈时间和剂量依赖性表达。通过使用信号分子的各种抑制剂来阐明I-BOP诱导COX-2表达的信号通路。在蛋白质水平、酶活性和COX-2启动子活性方面评估这些抑制剂的作用。在丝裂原活化蛋白激酶(MAPK)家族中,细胞外调节蛋白激酶(ERK)和p38 MAPK通路而非c-Jun氨基末端激酶/应激激活蛋白激酶(JNK/SAPK)通路参与了诱导过程。其他通路如Janus激酶/信号转导和转录激活因子3(JAK/Stat3)通路和β-连环蛋白/TCF/淋巴样增强因子(LEF)通路也参与了诱导。在磷酸化步骤进一步研究了参与COX-2转录的关键信号分子ERK、p38 MAPK、环磷腺苷反应元件结合蛋白(CREB)和核因子κB(NF-κB)的激活情况。ERK和p38 MAPK的激活似乎主要由表皮生长因子受体(EGFR)的反式激活介导,而CREB和NF-κB的激活由蛋白激酶A(PKA)、蛋白激酶C(PKC)和ERK介导。在启动子水平进一步探讨了CREB和NF-κB在I-BOP诱导COX-2表达中的作用。对启动子片段和反应基序突变的研究表明,CRE和NF-κB位点对COX-2的诱导至关重要。远端NF-κB位点对COX-2转录的基础诱导至关重要,而CRE和近端NF-κB位点对诱导转录很重要。这些结果表明,I-BOP通过多种信号通路诱导COX-2表达。

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