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Adenovirus-mediated N5 gene transfer inhibits tumor growth and metastasis of human carcinoma in nude mice

机译:腺病毒介导的N5基因转移抑制裸鼠人肿瘤的生长和转移

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The therapeutic effectiveness of cancer therapy often relies on induction of apoptotic cell death. Gene-therapy–mediated induction of apoptosis, therefore, may provide an effective means to kill cancer cells. The N5 gene encodes a death-domain–containing protein (p84N5) that can trigger atypical apoptosis from within the nucleus, suggesting it may be a candidate for use as a gene therapy for cancer. In the present study, we test the potential utility of a recombinant adenovirus designed to express the N5 gene(AdN5) for the treatment of a variety of human cancers using in vitro and animal models. In vitro, adenoviral-mediated N5gene transfer inhibits the growth of five different tumor cell lines, but not a normal diploid fibroblast cell line. Adenoviral-mediated N5gene transfer also reduces the growth and metastasis of primary human tumors in subcutaneous and orthotopic xenograft mouse models. Reduction in tumor cell growth in vitro and in vivo correlates with increased expression of p84N5 and induction of apoptosis. The relative sensitivity of different human cancer cells to AdN5 or Adp53 varies, suggesting that AdN5 may be effective in tumors relatively resistant to p53 gene therapy. We conclude that N5 has potential utility for the gene therapy of cancer.
机译:癌症疗法的治疗效果通常取决于诱导凋亡细胞死亡。因此,基因治疗介导的凋亡诱导可能提供杀死癌细胞的有效手段。 N5基因编码一个包含死亡域的蛋白质(p84N5),该蛋白质可以触发细胞核内的非典型凋亡,这表明它可能是癌症基因治疗的候选药物。在本研究中,我们测试使用体外和动物模型设计的表达N5基因的重组腺病毒(AdN5)的潜在用途,以治疗多种人类癌症。在体外,腺病毒介导的N5基因转移抑制了五种不同肿瘤细胞系的生长,但不抑制正常的二倍体成纤维细胞系的生长。在皮下和原位异种移植小鼠模型中,腺病毒介导的N5基因转移还减少了原发性人类肿瘤的生长和转移。体外和体内肿瘤细胞生长的减少与p84N5表达的增加和细胞凋亡的诱导有关。不同的人类癌细胞对AdN5或Adp53的相对敏感性各不相同,这表明AdN5可能在对p53基因治疗相对耐药的肿瘤中有效。我们得出结论,N5在癌症的基因治疗中具有潜在的实用性。

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