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Co-Assembly of Peptide with G-Quadruplex DNA: A Strategic Approach to Develop Anticancer Therapeutics

机译:肽与G-四链体DNA的共组装:开发抗癌疗法的战略方法

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摘要

G-quadruplex (G4) is one of the non-canonical nucleic acid structures that regulate multiple key biological processes. The formation of G4 hinders the progression of cancer. The molecular entities which can stabilize the G4 structure are very important to design anticancer therapeutics. Herein, it is described that a synthetic dendron-like peptide, C~(83)-(YYEE)-E co-assembles with G4 DNA in aqueous buffer containing Na~+ ions. Various orthogonal biophysical studies have established the co-assembly phenomenon. In silico, molecular docking studies also corroborate the results obtained from biophysical experiments. Importantly, the co-assembly enhances the thermal stability of G4 DNA compared to free G4 DNA. The peptide inhibits the activity of telomerase enzyme which is found to be over-expressed in most of the cancer cells and also down-regulates the c-Myc oncogenic expression. The peptide exhibits significant cytotoxic effect on cancer cells (HeLa and U2OS) compared to non-cancer cells (HEK293) under similar experimental conditions. The study highlights the applicability of a synthetic bioactive peptide as a putative anticancer therapeutic.
机译:G-quadruplex (G4)是一个非规范核酸结构调节多个关键的生物过程。阻碍了癌症的发展。实体可稳定G4结构非常重要的设计抗癌疗法。在此,它是合成的描述dendron-like肽C ~(83)——(YYEE) - eco-assembles G4 DNA在水缓冲包含Na ~ +离子。生物物理的研究建立了co-assembly现象。对接研究也证实结果从生物物理实验。重要的是,co-assembly增强热G4 DNA的稳定性比自由G4 DNA。肽抑制端粒酶的活性酶中发现过度大多数的癌细胞,但也下调原癌基因致癌表达式。展品重大癌症细胞毒性效应细胞(海拉和U2OS)而非癌症细胞(HEK293)类似的实验条件。合成生物活性肽的适用性一个假定的抗癌治疗。

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