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首页> 外文期刊>Journal of Medicinal Chemistry >Isaindigotone Derivatives: A New Class of Highly Selective Ligands for Telomeric G-Quadruplex DNA
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Isaindigotone Derivatives: A New Class of Highly Selective Ligands for Telomeric G-Quadruplex DNA

机译:Isaindigotone衍生物:一种新型的端粒G-四链体DNA的高选择性配体。

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Four isaindigotone derivatives (5a,b and 6a,b) designed as telomeric G-quadruplex ligands have been synthesized and characterized. The unfused aromatic rings in these compounds allow a flexible and adaptive conformation in G-quadruplex recognition. The interaction of human telomeric G-quadruplex DNA with these designed ligands was explored by means of FRET melting, fluorescence titration, CD spectroscopy, continuous variation; and molecular modeling studies. Our results showed that the adaptive scaffold might not only allow the ligands to well occupy the G-quartet but also perfectly bind to the grooves of the G-quadruplex. The synergetic effect of the multiple binding modes might be responsible for the improved binding ability and high selectivity of these ligands toward G-quadruplex over duplex DNA. Long-term exposure of HL60 and CA46 cancer cells to compound 5a showed a remarkable decrease in population growth, cellular senescence phenotype, and shortening of the telomere length, which is consistent with the behavior of an effective telomeric G-quadruplex ligand and telomerase inhibitor.
机译:合成并表征了四种设计为端粒G-四链体配体的异靛酮衍生物(5a,b和6a,b)。这些化合物中未融合的芳环在G-四链体识别中具有灵活且自适应的构象。通过FRET熔解,荧光滴定,CD光谱,连续变化等方法探索了人类端粒G-四链体DNA与这些设计的配体之间的相互作用。和分子建模研究。我们的研究结果表明,自适应支架不仅可以使配体很好地占据G四联体,而且可以与G四联体的凹槽完美结合。多种结合模式的协同作用可能是这些配体对双链DNA上的G-四链体的结合能力增强和选择性高的原因。 HL60和CA46癌细胞对化合物5a的长期暴露表明种群增长,细胞衰老表型和端粒长度缩短显着降低,这与有效端粒G-四链体配体和端粒酶抑制剂的行为一致。

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