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Induction of Connective Tissue Growth Factor Expression by Hypoxia in Human Lung Fibroblasts via the MEKK1/MEK1/ERK1/GLI-1/GLI-2 and AP-1 Pathways

机译：缺氧通过MEKK1 / MEK1 / ERK1 / GLI-1 / GLI-2和AP-1途径在人肺成纤维细胞中诱导结缔组织生长因子表达

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Several reports have indicated that hypoxia, GLI, and connective tissue growth factor (CTGF) contribute to pulmonary fibrosis in idiopathic pulmonary fibrosis. We investigated the participation of mitogen-activated protein kinase kinase (MEK) kinase 1 (MEKK1)/MEK1/ERK1/GLI-1/2 and activator protein-1 (AP-1) signaling in hypoxia-induced CTGF expression in human lung fibroblasts. Hypoxia time-dependently increased CTGF expression, which was attenuated by the small interfering RNA (siRNA) of GLI-1 (GLI-1 siRNA) and GLI-2 (GLI-2 siRNA) in both human lung fibroblast cell line (WI-38) and primary human lung fibroblasts (NHLFs). Moreover, GLI-1 siRNA and GLI-2 siRNA attenuated hypoxia-induced CTGF-luciferase activity, and the treatment of cells with hypoxia induced GLI-1 and GLI-2 translocation. Furthermore, hypoxia-induced CTGF expression was reduced by an MEK inhibitor (PD98059), MEK1 siRNA, ERK inhibitor (U0126), ERK1 siRNA, and MEKK1 siRNA. Both PD98059 and U0126 significantly attenuated hypoxia-induced CTGF-luciferase activity. Hypoxia time-dependently increased MEKK1, ERK, and p38 MAPK phosphorylation. Moreover, SB203580 (a p38 MAPK inhibitor) also apparently inhibited hypoxia-induced CTGF expression. The treatment of cells with hypoxia induced ERK, GLI-1, or GLI-2 complex formation. Hypoxia-induced GLI-1 and GLI-2 translocation into the nucleus was significantly attenuated by U0126. In addition, hypoxia-induced ERK Tyr204 phosphorylation was impeded by MEKK1 siRNA. Moreover, hypoxia-induced CTGF-luciferase activity was attenuated by cells transfected with AP-1 site mutation in a CTGF construct. Exposure to hypoxia caused a time-dependent phosphorylation of c-Jun, but not of c-Fos. Chromatin immunoprecipitation (ChIP) revealed that hypoxia induced the recruitment of c-Jun, GLI-1, and GLI-2 to the AP-1 promoter region of CTGF. Hypoxia-treated cells exhibited an increase in α-smooth muscle actin (α-SMA) and collagen production, which was blocked by GLI-1 siRNA and GLI-2 siRNA. Overall, these data implied that the MEKK1/MEK1/ERK1/GLI-1/GLI-2, and AP-1 pathways mediated hypoxia-induced CTGF expression in human lung fibroblasts. Furthermore, GLI-1 and GLI-2 found to be involved in hypoxia-induced α-SMA and collagen expression.

机译：几篇报道表明，低氧，GLI和结缔组织生长因子（CTGF）会导致特发性肺纤维化中的肺纤维化。我们调查了有丝分裂原激活的蛋白激酶激酶（MEK）激酶1（MEKK1）/ MEK1 / ERK1 / GLI-1 / 2和激活蛋白1（AP-1）信号参与缺氧诱导的人成纤维细胞CTGF表达。缺氧时间依赖性地增加了CTGF的表达，这被人肺成纤维细胞系（WI-38）中的GLI-1（GLI-1 siRNA）和GLI-2（GLI-2 siRNA）的小干扰RNA（siRNA）减弱了。）和原代人肺成纤维细胞（NHLF）。此外，GLI-1 siRNA和GLI-2 siRNA减弱了低氧诱导的CTGF荧光素酶活性，并用低氧诱导的GLI-1和GLI-2易位细胞进行了处理。此外，MEK抑制剂（PD98059），MEK1 siRNA，ERK抑制剂（U0126），ERK1 siRNA和MEKK1 siRNA降低了缺氧诱导的CTGF表达。 PD98059和U0126均显着减弱了缺氧诱导的CTGF荧光素酶活性。缺氧时间依赖性地增加了MEKK1，ERK和p38 MAPK磷酸化。此外，SB203580（p38 MAPK抑制剂）也明显抑制了缺氧诱导的CTGF表达。用缺氧处理细胞会诱导ERK，GLI-1或GLI-2复合物形成。缺氧诱导的GLI-1和GLI-2易位到核中，被U0126显着减弱。此外，缺氧诱导的ERK Tyr204磷酸化受到MEKK1 siRNA的阻碍。而且，低氧诱导的CTGF-荧光素酶活性被CTGF构建体中AP-1位点突变转染的细胞减弱。暴露于缺氧会引起c-Jun的时间依赖性磷酸化，但不会引起c-Fos的磷酸化。染色质免疫沉淀（ChIP）显示，低氧诱导c-Jun，GLI-1和GLI-2募集到CTGF的AP-1启动子区域。缺氧处理的细胞表现出α平滑肌肌动蛋白（α-SMA）和胶原蛋白生成的增加，这被GLI-1 siRNA和GLI-2 siRNA阻断。总体而言，这些数据表明，MEKK1 / MEK1 / ERK1 / GLI-1 / GLI-2和AP-1途径介导了缺氧诱导的人肺成纤维细胞CTGF表达。此外，发现GLI-1和GLI-2与低氧诱导的α-SMA和胶原蛋白表达有关。

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期刊名称 PLoS Clinical Trials
作者
Yi Cheng; Chien-huang Lin; Jing-Yun Chen; Chien-Hua Li; Yu-Tin Liu; Bing-Chang Chen;
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年(卷),期 2011(11),8
年度 2011
页码 e0160593
总页数 23
原文格式 PDF
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专利

1. Endothelin-1 induces connective tissue growth factor expression in human lung fibroblasts by ETAR-dependent JNK/AP-1 pathway [J] . WengC.-M., YuC.-C., KuoM.-L., Biochemical Pharmacology . 2014 ,第3期

机译：内皮素-1通过ETAR依赖的JNK / AP-1途径诱导人肺成纤维细胞中结缔组织生长因子的表达
2. Connective tissue growth factor induces collagen I expression in human lung fibroblasts through the Rac1/MLK3/JNK/AP-1 pathway [J] . LinC.-H., YuM.-C., TungW.-H., Biochimica et biophysica acta. Molecular cell research . 2013 ,第12期

机译：结缔组织生长因子通过Rac1 / MLK3 / JNK / AP-1途径诱导人肺成纤维细胞中胶原I的表达
3. Thrombin-Induced Connective Tissue Growth Factor Expression in Human Lung Fibroblasts Requires the ASK1/JNK/AP-1 Pathway [J] . Chung-Chi Yu, Ming-Jen Hsu, Min-Liang Kuo, The journal of immunology . 2009 ,第12期

机译：凝血酶诱导的人肺成纤维细胞结缔组织生长因子表达需要ASK1 / JNK / AP-1途径
4. Shear Stress Upregulates Human Fibroblast MAPK and Hypoxia Inducible Factor-1 Expression In Vitro [C] . Trindade MCD, Miyanishi K, Wang Z, Annual meeting of the Society For Biomaterials . 2003

机译：剪应力上调人成纤维细胞MAPK和缺氧诱导因子1的表达。
5. Signal transduction pathways mediating the expression of connective tissue growth factor by TGF[beta]1 in human gingival fibroblasts: Regulation by prostaglandin-E2. [D] . Black, Samuel Arthur, Jr. 2007

机译：TGFβ1介导人牙龈成纤维细胞中结缔组织生长因子表达的信号转导途径：由前列腺素-E2调节。
6. Correction: Induction of Connective Tissue Growth Factor Expression by Hypoxia in Human Lung Fibroblasts via the MEKK1/MEK1/ERK1/GLI-1/GLI-2 and AP-1 Pathways [O] . Yi Cheng, Chien-huang Lin, Jing-Yun Chen, 2011

机译：纠正：低氧通过MEKK1 / MEK1 / ERK1 / GLI-1 / GLI-2和AP-1途径在人肺成纤维细胞中诱导结缔组织生长因子表达
7. Correction: Induction of Connective Tissue Growth Factor Expression by Hypoxia in Human Lung Fibroblasts via the MEKK1/MEK1/ERK1/GLI-1/GLI-2 and AP-1 Pathways [O] . Yi Cheng, Chien-huang Lin, Jing-Yun Chen, 2017

机译：校正：通过MEKK1 / MEK1 / ERK1 / GLI-1 / GLI-2和AP-1途径诱导人肺成纤维细胞缺氧中缺氧的结缔组织生长因子表达

Induction of Connective Tissue Growth Factor Expression by Hypoxia in Human Lung Fibroblasts via the MEKK1/MEK1/ERK1/GLI-1/GLI-2 and AP-1 Pathways

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