Department of Biochemistry, Hebei Medical University, No. 361, Zhongshan East Road, Shijiazhuang 050017, China.
J Biochem. 2009 Nov;146(5):683-91. doi: 10.1093/jb/mvp115. Epub 2009 Jul 23.
Krüppel-like factor 5 (KLF5) and c-Jun are involved in angiotensin II (Ang II)-induced cell proliferation and play an important role in p21 expression. But the direct and functional implications of KLF5 and c-Jun in regulating p21 expression in vascular smooth muscle cells (VSMCs) are unclear. Here, we show that Ang II upregulated KLF5 and c-Jun expression and inhibited p21 expression in VSMCs, and silencing of KLF5 expression by KLF5-specific small interfering RNA (siRNA) neutralized the inhibitory effects of Ang II on p21 expression. Exposure of VSMCs to Ang II rapidly and strongly stimulated KLF5 phosphorylation, which results in an increase of the interaction of KLF5 with c-Jun. Treating VSMCs with PD98059, the ERK inhibitor, inhibited ERK activation and KLF5 phosphorylation as well as the interaction between KLF5 and c-Jun. Reporter analysis showed that both KLF5 and c-Jun cooperatively repressed the promoter of p21. Furthermore, KLF5 bound to its cis-elements in the p21 promoter, and meanwhile interacted with c-Jun in Ang II-induced VSMCs. These results suggest that Ang II induces KLF5 phosphorylation mediated by the ERK signalling in VSMCs, which in turn stimulates the interaction of KLF5 with c-Jun, subsequently leads to the suppression of p21 expression.
Krüppel 样因子 5(KLF5)和 c-Jun 参与血管紧张素 II(Ang II)诱导的细胞增殖,在 p21 表达中发挥重要作用。但是 KLF5 和 c-Jun 在调节血管平滑肌细胞(VSMCs)中 p21 表达中的直接和功能意义尚不清楚。在这里,我们发现 Ang II 上调了 KLF5 和 c-Jun 的表达,并抑制了 VSMCs 中的 p21 表达,而 KLF5 特异性小干扰 RNA(siRNA)沉默 KLF5 的表达则中和了 Ang II 对 p21 表达的抑制作用。Ang II 暴露可迅速且强烈地刺激 KLF5 磷酸化,从而增加 KLF5 与 c-Jun 的相互作用。用 ERK 抑制剂 PD98059 处理 VSMCs 可抑制 ERK 激活和 KLF5 磷酸化以及 KLF5 与 c-Jun 之间的相互作用。报告基因分析表明,KLF5 和 c-Jun 均协同抑制 p21 启动子。此外,KLF5 结合其 p21 启动子中的顺式元件,同时与 Ang II 诱导的 VSMCs 中的 c-Jun 相互作用。这些结果表明,Ang II 在 VSMCs 中诱导 ERK 信号转导的 KLF5 磷酸化,进而刺激 KLF5 与 c-Jun 的相互作用,从而导致 p21 表达的抑制。
