大黄酸哌嗪雌酚酮抑制人成骨样MG-63细胞分泌IL-6分子机制的研究

目的探讨大黄酸哌嗪雌酚酮(rhein-piperizinyl-estrone,命名为LC)调节人成骨样MG-63细胞分泌IL-6的分子机制。方法在原工作基础上,选择兼有2种雌激素受体(estrogen receptor,ER)亚型表达的人成骨样MG-63细胞为研究模型,采用ELISA、RT-PCR及荧光素酶报告基因检测、小RNA干扰及免疫印迹等技术,探讨LC对人成骨细胞产生的骨吸收调节因子IL-6表达的作用及作用机制。结果 LC可抑制MG-63细胞IL-6表达和IL-6基因启动子的转录活性,该作用可被纯ER阻断剂ICI182,780完全阻断,应用小RNA干扰技术进一步证实LC对成骨细胞IL-6产生的抑制作用是由ERα和ERβ共同介导的。PD98059(MEK1/2抑制剂)和Wortmannin(PI3K抑制剂)可分别阻断LC诱导的成骨细胞ERK和Akt的活化作用。结论 LC抑制成骨细胞产生IL-6是经ER途径、由ERα和ERβ共同介导的,LC还可通过活化Ras/MEK/ERK和PI3K/Akt信号通路对成骨细胞发挥作用。

Study on the molecular mechanism for inhibitory effects of rhein-piperizinyl-estrone on IL-6 secretion in human osteoblast-like MG-63 cells

This study aimed to investigate the molecular mechanism for inhibitory effect of rhein-piperizinyl-estrone(LC) on IL-6 secretion in human osteoblast-like MG-63 cells.Based on our previous studies,human osteoblast-like MG-63 cells containing two estrogen receptors(ER) isoforms were selected as model for this study.Enzyme-linked immnosorbent assay(ELISA),RT-PCR,luciferase reporter assay,small interfering double-stranded RNAs(siRNA) technology and Western blot were performed to investigate the effect of LC on IL-6 expression in osteoblast-derived cells and underline the molecular mechanism.We found that LC inhibited IL-6 expression and IL-6 promoter activity of human osteoblastic MG-63 cells.But treatment with the ER antagonist ICI 182,780 abrogated the above actions of LC on osteoblast-derived cells.In conclusion,the effects of LC on IL-6 production are mediated by both ERα and ERβ.Furthermore,LC functioned at least partially through activation of Ras/MEK/ERK and PI3K/Akt signaling.