Hong Jungil, Kwon Seok Joo, Sang Shengmin, Ju Jihyeung, Zhou Jian-nian, Ho Chi-Tang, Huang Mou-Tuan, Yang Chung S
Susan Lehman Cullman Laboratory for Cancer Research, Department of Chemical Biology, Ernest Mario School of Pharmacy, The State University of New Jersey, Piscataway, NJ 08854, USA.
Free Radic Biol Med. 2007 Apr 15;42(8):1211-21. doi: 10.1016/j.freeradbiomed.2007.01.016. Epub 2007 Jan 13.
Garcinol, a polyisoprenylated benzophenone, from the Garcinia indica fruit rind, has been suggested to be an anti-inflammatory and anti-cancer agent. To explore the possible use of this redox-sensitive compound as a colon cancer preventive agent, we investigated the effects of garcinol and its oxidative derivatives, cambogin, garcim-1, and garcim-2, on the growth of HT-29 and HCT-116 colon cancer cells, as well as IEC-6 and INT-407 normal immortalized intestinal cells. Garcinol and its derivatives showed potent growth-inhibitory effects on all intestinal cells, showing IC50 of 3.2-21.4 microM after a 3-day treatment. Garcim-1 exhibited the strongest effect with IC50 of 3.2-5.9 microM. Garcinol was more effective in inhibiting growth of cancer cells than that of normal immortalized cells. Flow-cytometric analysis showed increased sub-G1 cells by treatment with garcinol and cambogin. Induction of apoptosis by garcinol and cambogin (2-10 microM) was also observed based on caspase-3 activation and enhanced annexin V staining. The inhibitory effect of garcinol on cell growth was much more pronounced in the absence of fetal bovine serum (FBS), decreasing IC50 to 1.5 from 11.8 microM in 72-h incubations and to 3 from 38 microM in 24-h incubations, possibly due to the binding of garcinol to FBS, which markedly reduced cellular levels of garcinol. Under these conditions, redox reactions seem not to be involved in the inhibition. In contrast to the inhibitory effect, low concentrations (<1 microM) of garcinol and cambogin stimulated the growth of both normal and cancer cells by 10-100%, and the activity seemed to be mediated by reactive oxygen species. In the presence of superoxide dismutase/catalase or N-acetyl cysteine, low concentrations of garcinol (<1 microM) decreased cell growth. Garcinol (0.5-1 microM) also increased the phosphorylation of extracellular signal-related kinase 1/2 and AKT and the level of survivin, and the effects were abolished in the presence of superoxide dismutase/catalase. Our results indicate that garcinol and its derivatives can inhibit intestinal cell growth, but low concentrations of garcinol can stimulate cell growth. It remains to be determined whether the currently observed stimulatory and inhibitory effects of garcinol on colon cell growth occur in vivo.
藤黄脂素是一种来自印度藤黄果壳的聚异戊烯基化二苯甲酮,被认为是一种抗炎和抗癌剂。为了探索这种氧化还原敏感化合物作为结肠癌预防剂的可能用途,我们研究了藤黄脂素及其氧化衍生物藤黄精、藤黄脂素-1和藤黄脂素-2对HT-29和HCT-116结肠癌细胞以及IEC-6和INT-407正常永生化肠细胞生长的影响。藤黄脂素及其衍生物对所有肠细胞均显示出强大的生长抑制作用,3天处理后的IC50为3.2 - 21.4微摩尔。藤黄脂素-1表现出最强的作用,IC50为3.2 - 5.9微摩尔。藤黄脂素在抑制癌细胞生长方面比正常永生化细胞更有效。流式细胞术分析显示,用藤黄脂素和藤黄精处理后,亚G1期细胞增加。基于半胱天冬酶-3激活和膜联蛋白V染色增强,还观察到藤黄脂素和藤黄精(2 - 10微摩尔)诱导细胞凋亡。在无胎牛血清(FBS)的情况下,藤黄脂素对细胞生长的抑制作用更为明显,在72小时孵育中IC50从11.8微摩尔降至1.5微摩尔,在24小时孵育中从38微摩尔降至3微摩尔,这可能是由于藤黄脂素与FBS结合,显著降低了细胞内藤黄脂素水平。在这些条件下,氧化还原反应似乎不参与抑制作用。与抑制作用相反,低浓度(<1微摩尔)的藤黄脂素和藤黄精使正常细胞和癌细胞的生长均增加了10% - 100%,且该活性似乎由活性氧介导。在存在超氧化物歧化酶/过氧化氢酶或N-乙酰半胱氨酸的情况下,低浓度的藤黄脂素(<1微摩尔)会降低细胞生长。藤黄脂素(0.5 - 1微摩尔)还增加了细胞外信号调节激酶1/2和AKT的磷酸化以及生存素水平,而在存在超氧化物歧化酶/过氧化氢酶的情况下这些作用被消除。我们的结果表明,藤黄脂素及其衍生物可以抑制肠细胞生长,但低浓度的藤黄脂素可以刺激细胞生长。藤黄脂素目前观察到的对结肠细胞生长的刺激和抑制作用是否在体内发生仍有待确定。
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