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Potent antitumor efficacy of XAF1 delivered by conditionally replicative adenovirus vector via caspase-independent apoptosis

机译:有条件复制的腺病毒载体通过不依赖胱天蛋白酶的细胞凋亡提供的XAF1的强抗肿瘤功效

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XAF1 is a newly identified tumor-suppressor gene that can antagonize XIAP and sensitize cells to other cell death triggers. In this study, we utilized ZD55, a conditionally replicative adenovirus (CRAd) similar to ONYX-015 as the vector to transfer XAF1 into the tumor cells to evaluate its antitumor efficacy in vitro and in vivo. Potent and specific cytopathic effect (CPE) was observed upon infection with ZD55-XAF1 in tumor cell lines. Importantly, ZD55-XAF1 exhibited a superior suppression of tumor growth in an animal model of colorectal carcinoma in nude mice compared with Ad-XAF1 (E1-deleted replication-defective viral) and ONYX-015. Complete eradication of the established tumors was observed in four of eight mice. Our data also showed that infection with ZD55-XAF1 resulted in caspase-independent apoptosis. Although caspase-3, poly(ADP-ribose) polymerase were mildly activated in response to ZD55-XAF1 infection, pretreatment with pan-caspase inhibitor hardly influence its apoptosis-inducing activity. In summary, our study strongly suggested that ZD55-XAF1 could serve as an effective gene-virotherapy strategy and has highly potential against human cancers.
机译:XAF1是新近鉴定出的肿瘤抑制基因,可以拮抗XIAP并使细胞对其他细胞死亡触发物敏感。在这项研究中,我们利用ZD55(一种类似于ONYX-015的条件复制腺病毒(CRAd))作为载体将XAF1转移到肿瘤细胞中,以评估其在体内和体外的抗肿瘤功效。在肿瘤细胞系中感染ZD55-XAF1后,观察到了强力和特异的细胞病变作用(CPE)。重要的是,与Ad-XAF1(E1缺失的复制缺陷型病毒)和ONYX-015相比,ZD55-XAF1在裸鼠大肠癌动物模型中显示出对肿瘤生长的优异抑制作用。在八只小鼠中的四只中观察到完全根除已建立的肿瘤。我们的数据还显示,感染ZD55-XAF1会导致caspase依赖性凋亡。尽管响应ZD55-XAF1感染轻度激活了caspase-3,聚(ADP-核糖)聚合酶,但用pan-caspase抑制剂预处理几乎不会影响其凋亡诱导活性。总而言之,我们的研究强烈建议ZD55-XAF1可以作为一种有效的基因-病毒治疗策略,对人类癌症具有很高的潜力。

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