Dependence of Proximal GC Boxes and Binding Transcription Factors in the Regulation of Basal and Valproic Acid-Induced Expression of t-PA

IF 2.5 Q2 PERIPHERAL VASCULAR DISEASE International Journal of Vascular Medicine Pub Date : 2016-02-07 DOI:10.1155/2016/7928681
E. Ulfhammer, P. Larsson, Mia Magnusson, L. Karlsson, N. Bergh, S. Jern
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引用次数: 3

Abstract

Objective. Endothelial tissue-type plasminogen activator (t-PA) release is a pivotal response to protect the circulation from occluding thrombosis. We have shown that the t-PA gene is epigenetically regulated and greatly induced by the histone deacetylase (HDAC) inhibitor valproic acid (VPA). We now investigated involvement of known t-PA promoter regulatory elements and evaluated dependence of potential interacting transcription factors/cofactors. Methods. A reporter vector with an insert, separately mutated at either the t-PA promoter CRE or GC box II or GC box III elements, was transfected into HT-1080 and HUVECs and challenged with VPA. HUVECs were targeted with siRNA against histone acetyl transferases (HAT) and selected transcription factors from the Sp/KLF family. Results. An intact VPA-response was observed with CRE mutated constructs, whereas mutation of GC boxes II and III reduced the magnitude of the induction by 54 and 79% in HT-1080 and 49 and 50% in HUVECs, respectively. An attenuated induction of t-PA mRNA was observed after Sp2, Sp4, and KLF5 depletion. KLF2 and p300 (HAT) were identified as positive regulators of basal t-PA expression and Sp4 and KLF9 as repressors. Conclusion. VPA-induced t-PA expression is dependent on the proximal GC boxes in the t-PA promoter and may involve interactions with Sp2, Sp4, and KLF5.
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近端GC盒和结合转录因子在基础和丙戊酸诱导的t-PA表达调控中的依赖性
目标。内皮组织型纤溶酶原激活剂(t-PA)释放是保护血液循环免受血栓形成的关键反应。我们已经证明t-PA基因受表观遗传调控,并受到组蛋白去乙酰化酶(HDAC)抑制剂丙戊酸(VPA)的极大诱导。我们现在研究了已知的t-PA启动子调控元件的参与,并评估了潜在的相互作用转录因子/辅因子的依赖性。方法。将插入t-PA启动子CRE或GC box II或GC box III元件分别突变的报告载体转染到HT-1080和HUVECs中,并用VPA攻毒。HUVECs用siRNA靶向组蛋白乙酰转移酶(HAT)和来自Sp/KLF家族的转录因子。结果。在CRE突变构建体中观察到完整的vpa反应,而GC盒II和III的突变在HT-1080中分别降低了54%和79%,在HUVECs中分别降低了49%和50%。在Sp2、Sp4和KLF5缺失后,t-PA mRNA的诱导减弱。KLF2和p300 (HAT)是基础t-PA表达的阳性调节因子,Sp4和KLF9是抑制因子。结论。vpa诱导的t-PA表达依赖于t-PA启动子的近端GC盒,可能涉及与Sp2、Sp4和KLF5的相互作用。
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来源期刊
International Journal of Vascular Medicine
International Journal of Vascular Medicine PERIPHERAL VASCULAR DISEASE-
CiteScore
3.50
自引率
0.00%
发文量
7
审稿时长
16 weeks
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