Na Hye-Kyung, Surh Young-Joon
National Research Laboratory of Molecular Carcinogenesis and Chemoprevention, College of Pharmacy, Seoul National University, Seoul 151-742, South Korea.
Asia Pac J Clin Nutr. 2008;17 Suppl 1:204-7.
We previously reported that a novel alkylphospholipid type antitumor agent edelfosine (ET-18-O-CH3 ; 1-O-octadecyl-2-O-methyl-glycero-3-phosphocholine) induced apoptosis in human breast epithelial cells transfected with the H-ras oncogene (MCF10A-ras) which was causally linked to cyclooxygenase-2 (COX-2) up-regulation and production of 15-deoxy-Delta 12,14-prostaglandins J2 (15d-PGJ2). ET-18-O-CH3 treatment also enhanced the production of prostaglandin E2 (PGE2), a major COX-2 product. In this study, we found that ET-18-O-CH3 treatment resulted in elevated mRNA expression of the PGE2 receptor subunit, EP2 receptor. Exogenously added PGE2 inhibited the growth of MCF10A-ras cells and induced proteolytic cleavage of caspase 3. ET-18-O-CH3 also inhibited constitutive activation of ERK1/2, p38 MAPK, and Akt/protein kinase B, which was blunted by a selective COX-2 inhibitor SC58635. In addition, ET-18-O-CH3 inhibited DNA binding activity of NF-kappa B in MCF10A-ras cells, and this was again attenuated by SC58635. Based on these findings, it is likely that ET-18-O-CH3 inactivates ERK1/2, Akt, and NF-kappaB signaling via COX-2 induction in MCF10A-ras cells, thereby inducing apoptosis of these cells.
我们之前报道过,一种新型烷基磷脂类抗肿瘤药物依地福新(ET-18-O-CH3;1-O-十八烷基-2-O-甲基甘油-3-磷酸胆碱)可诱导转染了H-ras癌基因的人乳腺上皮细胞(MCF10A-ras)发生凋亡,这与环氧合酶-2(COX-2)上调及15-脱氧-Δ12,14-前列腺素J2(15d-PGJ2)的产生存在因果关系。ET-18-O-CH3处理还增强了主要的COX-2产物前列腺素E2(PGE2)的产生。在本研究中,我们发现ET-18-O-CH3处理导致PGE2受体亚基EP2受体的mRNA表达升高。外源添加的PGE2抑制了MCF10A-ras细胞的生长并诱导了半胱天冬酶3的蛋白水解切割。ET-18-O-CH3还抑制了ERK1/2、p38丝裂原活化蛋白激酶和Akt/蛋白激酶B的组成性激活,而选择性COX-2抑制剂SC58635可减弱这种抑制作用。此外,ET-18-O-CH3抑制了MCF10A-ras细胞中NF-κB的DNA结合活性,而SC58635再次减弱了这种抑制作用。基于这些发现,ET-18-O-CH3很可能通过在MCF10A-ras细胞中诱导COX-2使ERK1/2、Akt和NF-κB信号失活,从而诱导这些细胞凋亡。
