Fimognari Carmela, Sangiorgi Luca, Capponcelli Silvia, Nüsse Michael, Fontanesi Silvia, Berti Fausto, Soddu Silvia, Cantelli-Forti Giorgio, Hrelia Patrizia
Department of Pharmacology, University of Bologna, via Irnerio 48, 40126, Bologna, Italy.
Invest New Drugs. 2005 Jun;23(3):195-203. doi: 10.1007/s10637-005-6727-y.
We investigated apoptosis induction by sulforaphane on three cell lines characterized by a different p53 status. In particular, we used p53-knock-out fibroblasts from newborn mice transfected with the p53-Ser220 mutation, observed in Li-Fraumeni Syndrome patients, as a model of mutated p53 status. Moreover, immortalized fibroblasts from newborn mice expressing or lacking p53 (p53 +/+ and p53-/-, respectively) have been used to verify whether mutated p53 status could prevent sulforaphane-induced apoptotic events. Sulforaphane was able to induce apoptosis on all three cell lines. Indeed, the caspase-3 assays and poly(ADP-ribose)polymerase (PARP) cleavage data indicated that sulforaphane stimulated caspase-3-like activity and degradation of PARP. However, cells with a wild-type or mutated p53 appeared to be more sensitive to the effects of sulforaphane than cells lacking p53. Taken together, our results suggest that sulforaphane could act by a p53-independent pathway. For this reason, sulforaphane can be viewed as a novel agent useful not only in the treatment of Li-Fraumeni-associated tumors but also drug resistant tumors where p53 dysregulation is a feature.
我们研究了萝卜硫素对三种具有不同p53状态的细胞系的凋亡诱导作用。具体而言,我们使用了来自新生小鼠的p53基因敲除成纤维细胞,这些细胞转染了在李-佛美尼综合征患者中观察到的p53-Ser220突变,作为p53突变状态的模型。此外,来自新生小鼠的表达或缺失p53的永生化成纤维细胞(分别为p53 +/+和p53 -/-)已被用于验证突变的p53状态是否能阻止萝卜硫素诱导的凋亡事件。萝卜硫素能够在所有三种细胞系上诱导凋亡。实际上,半胱天冬酶-3检测和聚(ADP-核糖)聚合酶(PARP)裂解数据表明,萝卜硫素刺激了半胱天冬酶-3样活性和PARP的降解。然而,具有野生型或突变型p53的细胞似乎比缺乏p53的细胞对萝卜硫素的作用更敏感。综上所述,我们的结果表明萝卜硫素可能通过一条不依赖p53的途径起作用。因此,萝卜硫素可被视为一种新型药物,不仅可用于治疗与李-佛美尼综合征相关的肿瘤,还可用于治疗以p53失调为特征的耐药肿瘤。
