低聚物长度和碱基取代对人白血病CCRF-CEM细胞系GTn寡核苷酸细胞毒活性和特异性核蛋白识别的影响

C Morassutti, B Dapas, B Scaggiante, G Paroni, L Xodo, F Quadrifoglio
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引用次数: 11

摘要

我们已经鉴定出由G和T碱基组成的磷酸二酯寡核苷酸,命名为GTn,它能够通过识别特定的核蛋白来抑制人类癌细胞系的细胞生长。我们证明GTn寡核苷酸需要至少20个核苷酸的长度才能发挥显著的细胞毒作用并保持特定的蛋白质结合能力。此外,我们发现当在GTn序列的3'和5'端或内部引入A或C碱基时,GTn的细胞毒性丧失。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effect of oligomer length and base substitutions on the cytotoxic activity and specific nuclear protein recognition of GTn oligonucleotides in the human leukemic CCRF-CEM cell line.

We have identified phosphodiester oligonucleotides composed of G and T bases, named GTn, which are able to inhibit the cellular growth of human cancer cell lines by recognising specific nuclear proteins. We demonstrated that GTn oligonucleotides require a length of at least 20 nucleotides in order to exert a significant cytotoxic effect and to retain the specific protein binding ability. In addition, we found that GTn cytotoxicity was lost when A or C bases were introduced at either 3' and 5' end or within the GTn sequences.

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