YB-1 binds to the MMP-13 promoter sequence and represses MMP-13 transactivation via the AP-1 site

Shaija Samuel , Katherine K. Beifuss , Lori R. Bernstein
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引用次数: 24

Abstract

Matrix metalloproteinases (MMPs) are key enzymes that implement degradation of the extracellular matrix during cellular invasion in development, tissue remodeling, and pathogenic disease states. MMP-13 has pivotal roles in the pathogenesis of invasive cancers and arthritis. Here we report the identification of Y-box binding protein-1 (YB-1) as a new repressor of MMP-13 transactivation. YB-1 binds in vitro in DNA affinity chromatography to the activator protein-1 (AP-1) DNA sequence within the MMP-13 promoter. Chromatin immunoprecipitation assays reveal that YB-1 binds in living cells to the MMP-13 gene promoter to a region of the MMP-13 promoter containing the AP-1 site. YB-1 represses tumor promoter-induced MMP-13 promoter transactivation at the AP-1 site. This is the first report demonstrating YB-1 binding in vitro and in living cells to a mammalian AP-1 target gene, and the first report of YB-1 regulation of the MMP-13 promoter.

YB-1与MMP-13启动子序列结合,通过AP-1位点抑制MMP-13的转激活
基质金属蛋白酶(Matrix metalloproteinases, MMPs)是在细胞侵袭发育、组织重塑和致病性疾病状态中实现细胞外基质降解的关键酶。MMP-13在侵袭性癌症和关节炎的发病机制中起关键作用。在这里,我们报道了Y-box结合蛋白-1 (YB-1)作为MMP-13转录激活的新抑制因子的鉴定。在DNA亲和层析中,YB-1在体外与MMP-13启动子内的激活蛋白-1 (AP-1) DNA序列结合。染色质免疫沉淀实验显示,YB-1在活细胞中结合到MMP-13基因启动子上含有AP-1位点的区域。YB-1在AP-1位点抑制肿瘤启动子诱导的MMP-13启动子的转激活。这是首次在体外和活细胞中证实YB-1与哺乳动物AP-1靶基因结合的报道,也是首次报道YB-1调控MMP-13启动子。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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