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Plasmid-based Survivin shRNA and GRIM-19 carried by attenuated Salmonella suppresses tumor cell growth

机译:减毒沙门氏菌携带的基于质粒的Survivin shRNA和GRIM-19抑制肿瘤细胞生长

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摘要

Persistent activation of Survivin and its overexpression contribute to the formation, progression and metastasis of several different tumor types. Therefore, Survivin is an ideal target for RNA interference mediated-growth inhibition. Blockade of Survivin using specific short hairpin RNAs (shRNA) can significantly reduce prostate tumor growth. RNA interference does not fully ablate target gene expression, owing to the idiosyncrasies associated with shRNAs and their targets. To enhance the therapeutic efficacy of Survivin-specific shRNA, we employed a combinatorial expression of Survivin-specific shRNA and gene associated with retinoid-interferon-induced mortality-19 (GRIM-19). Then, the GRIM-19 coding sequences and Survivin-specific shRNAs were used to create a dual expression plasmid vector and were carried by an attenuated strain of Salmonella enteric serovar typhimurium (S. typhimurium) to treat prostate cancer in vitro and in vivo. We found that the co-expressed Survivin-specific shRNA and GRIM-19 synergistically and more effectively inhibited prostate tumor proliferation and survival, when compared with treatment with either single agent alone in vitro and in vivo. This study has provided a novel cancer gene therapeutic approach for prostate cancer.
机译:Survivin的持续活化及其过度表达有助于几种不同肿瘤类型的形成,发展和转移。因此,Survivin是RNA干扰介导的生长抑制的理想靶标。使用特定的短发夹RNA(shRNA)阻断Survivin可以显着降低前列腺肿瘤的生长。由于与shRNA及其靶标相关的特质,RNA干扰不能完全消除靶标基因的表达。为了增强Survivin特异的shRNA的治疗功效,我们采用了Survivin特异的shRNA和类维生素A干扰素诱导的死亡率19(GRIM-19)相关基因的组合表达。然后,使用GRIM-19编码序列和Survivin特异性shRNA构建双表达质粒载体,并由沙门氏菌肠型鼠伤寒鼠伤寒沙门氏菌(S. typhimurium)减毒株携带,以在体内和体外治疗前列腺癌。我们发现与单独在体外和体内使用任何一种药物进行治疗相比,共表达的Survivin特异性shRNA和GRIM-19协同且更有效地抑制了前列腺肿瘤的增殖和存活。这项研究为前列腺癌提供了一种新颖的癌症基因治疗方法。

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