抗炎咔唑LCY-2-CHO通过抑制巨噬细胞中p38丝裂原活化蛋白激酶信号通路来抑制脂多糖诱导的炎症介质表达。
The anti-inflammatory carbazole, LCY-2-CHO, inhibits lipopolysaccharide-induced inflammatory mediator expression through inhibition of the p38 mitogen-activated protein kinase signaling pathway in macrophages.
作者信息
Ho Feng-Ming, Lai Chih-Chang, Huang Li-Jiau, Kuo Tsun Cheng, Chao Chien M, Lin Wan-Wan
机构信息
Department of Internal Medicine, Tao-Yuan General Hospital, Department of Health, the Executive Yuan, Taiwan.
出版信息
Br J Pharmacol. 2004 Mar;141(6):1037-47. doi: 10.1038/sj.bjp.0705700. Epub 2004 Feb 23.
Abstract
- The present study was undertaken to investigate the anti-inflammatory effects of a synthetic compound, LCY-2-CHO, on the expression of inducible nitric oxide synthase (iNOS), COX-2, and TNF-alpha in murine RAW264.7 macrophages. 2. Within 1-30 microm, LCY-2-CHO concentration-dependently inhibited lipopolysaccharide (LPS)-induced nitric oxide (NO), prostaglandin E(2) (PGE(2)), and tumor necrosis factor-alpha (TNF-alpha) formation, with IC(50) values of 2.3, 1, and 0.8 microm, respectively. Accompanying inhibition of LPS-induced iNOS, cyclooxygenase-2 (COX-2), and pro-TNF-alpha proteins was observed. 3. Reverse transcription-polymerase chain reaction (RT-PCR) and promoter analyses indicated that iNOS expression was inhibited at the transcriptional level (IC(50)=2.3 microm), that inhibition of COX-2 expression only partially depended on gene transcription (IC(50)=7.6 microm), and that TNF-alpha transcription was unaffected. 4. Transcriptional assays revealed that activation of AP-1, but not NF-kappaB, was concomitantly blocked by LCY-2-CHO. Our results showed that LCY-2-CHO was capable of interfering with post-transcriptional regulation, altering the stability of COX-2 and TNF-alpha mRNAs. 5. Since the 3'-untranslated region (3' UTR) of both COX-2 and TNF-alpha mRNA contains a p38 mitogen-activated protein kinase (MAPK)-regulated element involved in mRNA stability, we assessed the effect of LCY-2-CHO on p38 MAPK. Our data clearly indicated an inhibition (IC(50)=1.7 microm) of LPS-mediated p38 MAPK activity, but not of extracellular signal-regulated kinase (ERK) or c-Jun N-terminal kinase (JNK) activity. However, kinase assays ruled out a direct inhibition of p38 MAPK action. The selective p38 MAPK inhibitor, SB203580, inhibited the promoter activities of iNOS and COX-2 rather than that of TNF-alpha. 6. In conclusion, LCY-2-CHO downregulates inflammatory iNOS, COX-2, and TNF-alpha gene expression in macrophages through interfering with p38 MAPK and AP-1 activation.
摘要
- 本研究旨在探讨合成化合物LCY - 2 - CHO对小鼠RAW264.7巨噬细胞中诱导型一氧化氮合酶(iNOS)、环氧化酶 - 2(COX - 2)和肿瘤坏死因子 - α(TNF - α)表达的抗炎作用。2. 在1 - 30微摩尔范围内,LCY - 2 - CHO浓度依赖性地抑制脂多糖(LPS)诱导的一氧化氮(NO)、前列腺素E2(PGE2)和肿瘤坏死因子 - α(TNF - α)的形成,IC50值分别为2.3、1和0.8微摩尔。同时观察到LPS诱导的iNOS、环氧化酶 - 2(COX - 2)和前体TNF - α蛋白受到抑制。3. 逆转录 - 聚合酶链反应(RT - PCR)和启动子分析表明,iNOS表达在转录水平受到抑制(IC50 = 2.3微摩尔),COX - 2表达的抑制仅部分依赖于基因转录(IC50 = 7.6微摩尔),而TNF - α转录不受影响。4. 转录分析显示,LCY - 2 - CHO同时阻断AP - 1的激活,但不阻断NF - κB的激活。我们的结果表明,LCY - 2 - CHO能够干扰转录后调控,改变COX - 2和TNF - α mRNA的稳定性。5. 由于COX - 2和TNF - α mRNA的3'非翻译区(3'UTR)都含有一个参与mRNA稳定性的p38丝裂原活化蛋白激酶(MAPK)调节元件,我们评估了LCY - 2 - CHO对p38 MAPK的影响。我们的数据清楚地表明,LCY - 2 - CHO抑制(IC50 = 1.7微摩尔)LPS介导的p38 MAPK活性,但不抑制细胞外信号调节激酶(ERK)或c - Jun N末端激酶(JNK)活性。然而,激酶分析排除了对p38 MAPK作用的直接抑制。选择性p38 MAPK抑制剂SB203580抑制iNOS和COX - 2的启动子活性,而不抑制TNF - α的启动子活性。6. 总之,LCY - 2 - CHO通过干扰p38 MAPK和AP - 1的激活来下调巨噬细胞中炎性iNOS、COX - 2和TNF - α基因的表达。
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