首页> 外文期刊>International journal of oncology >Non-viral delivery of the connexin 43 gene with histone deacetylase inhibitor to human nasopharyngeal tumor cells enhances gene expression and inhibits in vivo tumor growth
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Non-viral delivery of the connexin 43 gene with histone deacetylase inhibitor to human nasopharyngeal tumor cells enhances gene expression and inhibits in vivo tumor growth

机译:连接蛋白43基因与组蛋白脱乙酰基酶抑制剂向人鼻咽肿瘤细胞的非病毒传递可增强基因表达并抑制体内肿瘤的生长

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Dysregulation of connexin expression is believed to have a role in carcinogenesis, because levels of connexin are reduced in various tumors. We examined the role of connexin 43 (Cx43) alone and combined with a histone deactylase (HDAC) inhibitor in tumor growth inhibition. The transfection of Cx43 plasmid DNA (pCMV-Cx43) into human nasopharyngeal cancer KB cells using folate-linked nanoparticles induced inhibition of cell growth. Cx43 induced a tumor suppressive effect via a gap junctional intercellular communication-independent mechanism. The transfection of pCMV- Cx43 along with an HDAC inhibitor, 4-phenylbutyrate (4-PB), enhanced Cx43 expression greatly in vitro, and inhibited significantly the tumor growth of KB cells and xenografts compared with that of pCMV-Cx43 alone. 4-PB induced increased expression of genes of DNA damage checkpoints and of apoptosis via the down-regulation of anti-apoptotic bcl-2 mRNA expression and up-regulation of the activity of the apoptosis-associated enzyme caspase-3/7. Thus, the amplified Cx43 expression by an antitumor agent, an HDAC inhibitor, may have great potential as a growth inhibitor for nasopharyngeal tumors.
机译:连接蛋白表达的失调被认为在致癌作用中起作用,因为在各种肿瘤中连接蛋白的水平降低。我们研究了单独的连接蛋白43(Cx43)的作用,并与组蛋白去乙酰化酶(HDAC)抑制剂结合在肿瘤生长抑制中的作用。使用叶酸连接的纳米颗粒将Cx43质粒DNA(pCMV-Cx43)转染到人鼻咽癌KB细胞中可诱导细胞生长抑制。 Cx43通过间隙连接细胞间通讯独立机制诱导肿瘤抑制作用。与单独的pCMV-Cx43相比,pCMV-Cx43与HDAC抑制剂4-苯基丁酸酯(4-PB)的转染在体外大大增强了Cx43的表达,并显着抑制了KB细胞和异种移植的肿瘤生长。 4-PB通过下调抗凋亡bcl-2 mRNA的表达和上调凋亡相关酶caspase-3 / 7的活性来诱导DNA损伤检查点和凋亡基因的表达增加。因此,由抗肿瘤剂HDAC抑制剂扩增的Cx43表达作为鼻咽肿瘤的生长抑制剂具有巨大潜力。

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