Shin Dong Yeok, Kim Gi Young, Kim Nam Deuk, Jung Jee Hyung, Kim Se-Kwon, Kang Ho Sung, Choi Yung Hyun
Department of Biochemistry, Dongeui University College of Oriental Medicine, Busan 614-052, Korea.
Oncol Rep. 2008 Feb;19(2):517-26.
The tumor suppressor protein p53 restricts proliferation in response to DNA damage or the deregulation of mitogenic oncogenes, by leading to the induction of various cell cycle checkpoints, apoptosis or cellular senescence. Consequently, p53 mutations increase cell proliferation and survival and in some settings promote genomic instability and resistance to certain anti-cancer drugs. It is very important to identify chemotherapeutic agents that activate in a p53-independent manner for the development of treatments for p53-deficient tumors. Pectenotoxin-2 (PTX-2), isolated from marine sponges has been reported to display significant cytotoxicity to p53-deficient cancer cell lines. In this study, we compared the anti-cancer activity of PTX-2 in order to further test the status of p53 using two well-known hepatocarcinoma cell lines, p53-deficient Hep3B and p53-wild-type HepG2. MTT assay indicated that Hep3B cells were highly susceptible, whereas HepG2 cells were more resistant to this compound which was connected with the induction of apoptotic cell death in p53-deficient Hep3B cells, though not in HepG2 cells. The apoptosis induced by PTX-2 in Hep3B cells was associated with the down-regulation of anti-apoptotic Bcl-2 members (Bcl-2 and Bcl-xL) and IAP family proteins, the up-regulation of pro-apoptotic Bax protein and tumor necrosis factor-related apoptosis-inducing ligand (TRAIL)-receptor 1/receptor 2 (DR4/DR5) and mitochondrial dysfunction. PTX-2 activated caspases (caspase-3, -8 and -9) and the blockade of caspase-3 activity by the caspase-3 inhibitor prevented the PTX-2-induced apoptosis in Hep3B cells. Additionally, the transcription factor early growth response-1 (Egr-1) gene was transcriptionally activated and the levels of non-steroidal anti-inflammatory drugs (NSAID)-activated gene-1 (NAG-1) protein were also elevated in PTX-2-treated Hep3B cells. Although further studies are needed to prove that an increased expression of Egr-1 by PTX-2 directly leads to NAG-1 induction and then apoptosis induction in p53-deficient Hep3B cells, the results of this study suggest that PTX-2 may be a good candidate for the development of a potential anti-tumorigenic agent in p53-deficient tumors.
肿瘤抑制蛋白p53通过诱导各种细胞周期检查点、细胞凋亡或细胞衰老,对DNA损伤或有丝分裂原癌基因的失调做出反应,从而限制细胞增殖。因此,p53突变会增加细胞增殖和存活,在某些情况下还会促进基因组不稳定和对某些抗癌药物的耐药性。识别以p53非依赖性方式激活的化疗药物对于开发p53缺陷肿瘤的治疗方法非常重要。从海洋海绵中分离出的pectenotoxin-2(PTX-2)已被报道对p53缺陷的癌细胞系具有显著的细胞毒性。在本研究中,我们比较了PTX-2的抗癌活性,以便使用两种著名的肝癌细胞系——p53缺陷的Hep3B和p53野生型的HepG2,进一步检测p53的状态。MTT试验表明,Hep3B细胞对该化合物高度敏感,而HepG2细胞对其更具抗性,这与p53缺陷的Hep3B细胞中凋亡性细胞死亡的诱导有关,而在HepG2细胞中则不然。PTX-2在Hep3B细胞中诱导的凋亡与抗凋亡Bcl-2家族成员(Bcl-2和Bcl-xL)和IAP家族蛋白的下调、促凋亡Bax蛋白和肿瘤坏死因子相关凋亡诱导配体(TRAIL)受体1/受体2(DR4/DR5)的上调以及线粒体功能障碍有关。PTX-2激活了半胱天冬酶(半胱天冬酶-3、-8和-9),半胱天冬酶-3抑制剂对半胱天冬酶-3活性的阻断阻止了PTX-2在Hep3B细胞中诱导的凋亡。此外,转录因子早期生长反应-1(Egr-1)基因在转录水平上被激活,在PTX-2处理的Hep3B细胞中,非甾体抗炎药(NSAID)激活基因-1(NAG-1)蛋白的水平也升高。尽管需要进一步研究来证明PTX-2诱导的Egr-1表达增加直接导致p53缺陷的Hep3B细胞中NAG-1的诱导,进而诱导凋亡,但本研究结果表明,PTX-2可能是开发p53缺陷肿瘤潜在抗肿瘤药物的良好候选物。
