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首页> 外文期刊>Nucleosides, nucleotides and nucleic acids >Binding of G-quadruplex-interactive agents to distinct G-quadruplexes induces different biological effects in MiaPaCa cells.
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Binding of G-quadruplex-interactive agents to distinct G-quadruplexes induces different biological effects in MiaPaCa cells.

机译:G-四链体相互作用剂与不同的G-四链体的结合在MiaPaCa细胞中诱导不同的生物学效应。

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Our previous studies have demonstrated the preference of telomestatin for intramolecular, rather than the intermolecular, G-quadruplex structures, while TiMPyP4 has selectivity for intermolecular over intramolecular G-quadruplex structures. However, it was not clear whether the difference in the selectivity between two different G-quadruplex-interactive agents could determine the corresponding biological effects in cultured human tumor cells. Here we evaluated the biological effects of both TMPyP4 and telomestatin in the human pancreatic carcinoma cell line (MiaPaCa) using subtoxic and cytotoxic concentrations. The cytotoxicity of these agents against MiaPaCa cells is quite different, and the IC50 of telomestatin (0.5 microM) is about 100 times less than that of TMPyP4 (50 microM). At IC50 concentrations, TMPyP4 induced anaphase bridge formation in MiaPaCa cells, while telomestatin failed to induce anaphase bridge formation. At subtoxic concentrations, TMPyP4 induced MiaPaCa cell growth arrest, senescence, apoptosis, and telomere length shortening within 5 weeks, while similar biological effects were evident after 12 weeks following treatment with telomestatin. Our data suggest that binding of G-quadruplex-interactive agents to distinct G-quadruplexes could induce different biological effects in human cancer cells.
机译:我们以前的研究表明,端粒他汀对分子内而非分子间G-四链体结构的偏爱,而TiMPyP4对分子间而非分子内G-四链体结构具有选择性。然而,尚不清楚两种不同的G-四链体相互作用剂之间选择性的差异是否可以确定培养的人肿瘤细胞中的相应生物学效应。在这里,我们使用亚毒性和细胞毒性浓度评估了TMPyP4和端粒他汀在人胰腺癌细胞系(MiaPaCa)中的生物学作用。这些药物对MiaPaCa细胞的细胞毒性完全不同,端粒他汀(0.5 microM)的IC50比TMPyP4(50 microM)低约100倍。在IC50浓度下,TMPyP4诱导了MiaPaCa细胞的后期桥形成,而端粒他汀未能诱导后期桥形成。在亚毒性浓度下,TMPyP4诱导的MiaPaCa细胞生长停滞,衰老,凋亡和端粒长度在5周内缩短,而在用端粒他汀治疗12周后,相似的生物学效应也很明显。我们的数据表明,G-四链体相互作用剂与不同的G-四链体结合可以在人类癌细胞中诱导不同的生物学效应。

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