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Short hairpin RNA targeting survivin inhibits growth and angiogenesis of glioma U251 cells

机译:靶向survivin的短发夹RNA抑制神经胶质瘤U251细胞的生长和血管生成

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Survivin is a novel tumor-associated gene, its overexpression mostly associates with carcinogenesis and development. Nevertheless, the precise role of survivin in initiation and progression of gliomas is still not completely clear. We constructed here three short hairpin RNA (shRNA) targeting survivin plasmid vectors and introduced them into glioma U251 cells. The three shRNAs were efficiently and specifically able to knockdown the survivin expression in transiently transfected U251 cells. The stable transfectants expressing the shRNA having the strongest inhibitory effect against survivin exhibited decreased cell growth, increased spontaneous apoptosis, mitotic catastrophe and cell cycle arrest. Furthermore, in nude mice xenografts, the stable transfectants presented decreased de novo glioma formation and reduced development of angiogenesis. Results from this study indicate that survivin plays an important role in malignant proliferation, antiapoptosis and angiogenesis of gliomas, which may become an attractive target for gene therapy of gliomas, while RNA interference (RNAi) mediated by shRNA may become a new promising strategy for cancer gene therapy.
机译:Survivin是一个新的肿瘤相关基因,其过表达主要与癌变和发展有关。然而,survivin在神经胶质瘤的发生和发展中的确切作用尚不完全清楚。我们在这里构建了三个靶向survivin质粒载体的短发夹RNA(shRNA),并将其引入神经胶质瘤U251细胞。这三个shRNA能够有效且特异性地敲除瞬时转染的U251细胞中的survivin表达。表达对survivin抑制作用最强的shRNA的稳定转染子表现出细胞生长减少,自发凋亡增加,有丝分裂灾难和细胞周期停滞。此外,在裸鼠异种移植物中,稳定的转染子呈现出减少的新生神经胶质瘤形成和减少的血管生成。这项研究的结果表明,survivin在神经胶质瘤的恶性增殖,抗凋亡和血管生成中起着重要作用,这可能成为神经胶质瘤基因治疗的诱人靶标,而shRNA介导的RNA干扰(RNAi)可能成为新的有希望的癌症治疗策略。基因治疗。

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