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Uniquely modified RNA oligonucleotides targeting STAT3 suppress melanoma growth both in vitro andin vivo

机译:靶向STAT3的独特修饰的RNA寡核苷酸在体内外抑制黑色素瘤的生长

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摘要

Signal transducers and activators of transcription-3 (STAT3), a central cytoplasmic transcription factor, is frequently over-expressed and constitutively activated during malignant transformation. The overexpression of STAT3 in melanoma cells is often observed and is suggested to be involved in tumorigenesis and development. In this study, a novel antisense RNA oligonucleotides targeting the STAT3 mRNA was 2'-O-methyl modified with a 3'-butanol tag was designed, and found this uniquely modified strategy dramatic increased the stability of the RNA oligonucleotides.The results showed that the RNA oligonucleotides, namely STT-33 and STT-34, strongly inhibited the target gene expression in the melanoma cells and resulted in increase cell apoptosis. Furthermore, the RNA oligonucleotides could significantly inhibit melanoma cell proliferation and xenografts growth in nude mice.Thus, the novel modified RNA oligonucleotides targeting STAT3 may serve as a useful tool to study the involvement of STAT3 in melanoma and potentially as an anti-cancer agent for melanoma.
机译:信号转导和转录激活因子(STAT3)(一种中央细胞质转录因子)在恶性转化过程中经常过度表达并组成性激活。经常观察到STAT3在黑素瘤细胞中的过度表达,并提示其与肿瘤发生和发展有关。在这项研究中,设计了一种新的靶向STAT3 mRNA的反义RNA寡核苷酸,并用3'-丁醇标签进行了2'-O-甲基修饰,发现这种独特的修饰策略显着提高了RNA寡核苷酸的稳定性。 RNA寡核苷酸,即STT-33和STT-34,强烈抑制黑素瘤细胞中靶基因的表达,并导致细胞凋亡增加。此外,RNA寡核苷酸可显着抑制裸鼠黑色素瘤细胞的增殖和异种移植物的生长,因此,针对STAT3的新型修饰RNA寡核苷酸可能是研究STAT3参与黑色素瘤的有用工具,并可能作为抗癌剂黑色素瘤。

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