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ETS转录因子对间质胶原酶(MMP-1)基因表达的差异性调控

Differential regulation of interstitial collagenase (MMP-1) gene expression by ETS transcription factors.

作者信息

Westermarck J, Seth A, Kähäri V M

机构信息

Department of Dermatology, Turku University Central Hospital, Finland.

出版信息

Oncogene. 1997 Jun 5;14(22):2651-60. doi: 10.1038/sj.onc.1201111.

Abstract

Expression of interstitial collagenase (MMP-1) has been detected in stromal fibroblasts of various malignant tumors. Here, we have studied the effect of three structurally different ETS transcription factors (ETS-1, ERGB/Fli-1, and PU.1) on MMP-1 promoter activity in NIH3T3 fibroblasts. ETS-1 increased the activity of 3.8 kb MMP-1 promoter construct up to tenfold, while ERGB/Fli-1 or PU.1 alone had no marked effect on basal promoter activity. ETS-1 also markedly potentiated enhancement of MMP-1 promoter by both c-Jun and JunB, whereas ERGB/Fli-1 augmented only the effect of c-Jun. Interestingly, PU.1 abolished induction of MMP-1 promoter by both c-Jun and JunB. Stimulation of MMP-1 promoter by 12-O-tetradecanoyl phorbol-13-acetate and okadaic acid was differentially augmented by ETS-1 and ERGB/Fli-1, and abrogated by PU.1. Co-transfection studies with MMP-1 promoter 5'-deletion constructs revealed that AP-1 site was necessary for PU.1-elicited suppression. As compared to control cell lines, PU.1-positive stable cells exhibited clearly weaker binding of c-Jun and JunD containing AP-1 complexes to MMP-1 promoter AP-1 element, as well as marked reduction in basal level and induction of c-jun mRNA by 12-O-tetradecanoyl phorbol-13-acetate and okadaic acid, suggesting a novel mechanism for PU.1-mediated inhibition of AP-1 dependent gene expression. These results show that three structurally distinct ETS transcription factors differently modulate AP-1 dependent upregulation of MMP-1 gene expression.

摘要

在多种恶性肿瘤的基质成纤维细胞中已检测到间质胶原酶(MMP-1)的表达。在此,我们研究了三种结构不同的ETS转录因子(ETS-1、ERGB/Fli-1和PU.1)对NIH3T3成纤维细胞中MMP-1启动子活性的影响。ETS-1可使3.8 kb的MMP-1启动子构建体的活性增加至十倍,而单独的ERGB/Fli-1或PU.1对基础启动子活性没有明显影响。ETS-1还显著增强了c-Jun和JunB对MMP-1启动子的增强作用,而ERGB/Fli-1仅增强了c-Jun的作用。有趣的是,PU.1消除了c-Jun和JunB对MMP-1启动子的诱导作用。12-O-十四烷酰佛波醇-13-乙酸酯和冈田酸对MMP-1启动子的刺激作用在ETS-1和ERGB/Fli-1的作用下有差异地增强,而在PU.1的作用下被消除。与MMP-1启动子5'-缺失构建体的共转染研究表明,AP-1位点对于PU.1引发的抑制作用是必需的。与对照细胞系相比,PU.1阳性稳定细胞中含有c-Jun和JunD的AP-1复合物与MMP-1启动子AP-1元件的结合明显较弱,并且12-O-十四烷酰佛波醇-13-乙酸酯和冈田酸对c-jun mRNA基础水平的诱导作用也明显降低,这表明了PU.1介导的抑制AP-1依赖性基因表达的新机制。这些结果表明,三种结构不同的ETS转录因子对AP-1依赖性的MMP-1基因表达上调有不同的调节作用。

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