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三亚胺基五甲川菁衍生物与人类端粒 DNA G-四链体的相互作用。

Interactions Between Spermine-Derivatized Tentacle Porphyrins and The Human Telomeric DNA G-Quadruplex.

机构信息

Department of Chemistry and Biochemistry, Swarthmore College, Swarthmore, PA 19081, USA.

Lerner College of Medicine, Cleveland Clinic, Cleveland, OH 44195, USA.

出版信息

Int J Mol Sci. 2018 Nov 21;19(11):3686. doi: 10.3390/ijms19113686.

Abstract

G-rich DNA sequences have the potential to fold into non-canonical G-Quadruplex (GQ) structures implicated in aging and human diseases, notably cancers. Because stabilization of GQs at telomeres and oncogene promoters may prevent cancer, there is an interest in developing small molecules that selectively target GQs. Herein, we investigate the interactions of -tetrakis-(4-carboxysperminephenyl)porphyrin (TCPPSpm4) and its Zn(II) derivative (ZnTCPPSpm4) with human telomeric DNA (Tel22) via UV-Vis, circular dichroism (CD), and fluorescence spectroscopies, resonance light scattering (RLS), and fluorescence resonance energy transfer (FRET) assays. UV-Vis titrations reveal binding constants of 4.7 × 10⁶ and 1.4 × 10⁷ M and binding stoichiometry of 2⁻4:1 and 10⁻12:1 for TCPPSpm4 and ZnTCPPSpm4, respectively. High stoichiometry is supported by the Job plot data, CD titrations, and RLS data. FRET melting indicates that TCPPSpm4 stabilizes Tel22 by 36 ± 2 °C at 7.5 eq., and that ZnTCPPSpm4 stabilizes Tel22 by 33 ± 2 °C at ~20 eq.; at least 8 eq. of ZnTCPPSpm4 are required to achieve significant stabilization of Tel22, in agreement with its high binding stoichiometry. FRET competition studies show that both porphyrins are mildly selective for human telomeric GQ vs duplex DNA. Spectroscopic studies, combined, point to end-stacking and porphyrin self-association as major binding modes. This work advances our understanding of ligand interactions with GQ DNA.

摘要

富含 G 的 DNA 序列具有折叠成非典型 G-四链体 (GQ) 结构的潜力,这些结构与衰老和人类疾病有关,尤其是癌症。由于端粒和致癌基因启动子处 GQ 的稳定可能会阻止癌症的发生,因此人们有兴趣开发选择性靶向 GQ 的小分子。在此,我们通过紫外可见光谱、圆二色性 (CD) 和荧光光谱、共振光散射 (RLS) 和荧光共振能量转移 (FRET) 实验研究了 -四(4-羧基三亚甲基哌嗪基)卟啉 (TCPPSpm4) 和其 Zn(II) 衍生物 (ZnTCPPSpm4) 与人类端粒 DNA (Tel22) 的相互作用。紫外可见滴定表明,TCPPSpm4 和 ZnTCPPSpm4 的结合常数分别为 4.7×10⁶ 和 1.4×10⁷ M,结合比分别为 2-4:1 和 10-12:1。高结合比得到了 Job 图数据、CD 滴定和 RLS 数据的支持。FRET 熔融表明,TCPPSpm4 在 7.5 eq.时将 Tel22 稳定 36±2°C,而 ZnTCPPSpm4 在 ~20 eq.时将 Tel22 稳定 33±2°C;至少需要 8 eq.的 ZnTCPPSpm4 才能实现对 Tel22 的显著稳定,这与其高结合比一致。FRET 竞争研究表明,两种卟啉对人类端粒 GQ 与双链 DNA 都具有一定的选择性。综合光谱研究表明,末端堆积和卟啉自组装是主要的结合模式。这项工作加深了我们对配体与 GQ DNA 相互作用的理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1e05/6274827/066c93981999/ijms-19-03686-g001.jpg

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