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植物类黄酮非瑟酮优先靶向治疗相关 i-motif DNA 用于治疗应用。

Preferential targeting cancer-related i-motif DNAs by the plant flavonol fisetin for theranostics applications.

机构信息

FIBER (Frontier Institute for Biomolecular Engineering Research), Konan University, 7-1-20 Minatojima-Minamimachi, Chuo-ku, Kobe, 650-0047, Japan.

Department of Biophysics, Molecular Biology & Bioinformatics, University of Calcutta, University College of Science, 92, A.P.C. Road, Kolkata, 700009, India.

出版信息

Sci Rep. 2020 Feb 13;10(1):2504. doi: 10.1038/s41598-020-59343-2.

Abstract

The relationship of i-motif DNAs with cancer has prompted the development of specific ligands to detect and regulate their formation. Some plant flavonols show unique fluorescence and anti-cancer properties, which suggest the utility of the theranostics approach to cancer therapy related to i-motif DNA. We investigated the effect of the plant flavonol, fisetin (Fis), on the physicochemical property of i-motif DNAs. Binding of Fis to the i-motif from the promoter region of the human vascular endothelial growth factor (VEGF) gene dramatically induced the excited state intramolecular proton transfer (ESIPT) reaction that significantly enhanced the intensity of the tautomer emission band of Fis. This unique response was due to the coincidence of the structural change from i-motif to the hairpin-like structure which is stabilized via putative Watson-Crick base pairs between some guanines within the loop region of the i-motif and cytosines in the structure. As a result, the VEGF i-motif did not act as a replication block in the presence of Fis, which indicates the applicability of Fis for the regulation of gene expression of VEGF. The fluorescence and biological properties of Fis may be utilised for theranostics applications for cancers related to a specific cancer-related gene, such as VEGF.

摘要

i-motif DNA 与癌症的关系促使人们开发出特异性配体来检测和调节其形成。一些植物类黄酮具有独特的荧光和抗癌特性,这表明植物类黄酮作为治疗与 i-motif DNA 相关癌症的治疗方法具有一定的应用潜力。我们研究了植物类黄酮,漆黄素(Fis)对 i-motif DNA 理化性质的影响。Fis 与人类血管内皮生长因子(VEGF)基因启动子区 i-motif 的结合显著诱导了激发态分子内质子转移(ESIPT)反应,显著增强了 Fis 互变异构体发射带的强度。这种独特的响应归因于结构从 i-motif 到发夹样结构的变化,该结构通过 i-motif 环区中的一些鸟嘌呤与结构中胞嘧啶之间的可能 Watson-Crick 碱基对稳定。因此,在 Fis 的存在下,VEGF i-motif 不作为复制阻断物,这表明 Fis 可用于调节 VEGF 等特定与癌症相关基因的基因表达。Fis 的荧光和生物学特性可用于与特定癌症相关基因(如 VEGF)相关的癌症的治疗诊断应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b5f4/7018961/cf2ee0694607/41598_2020_59343_Fig1_HTML.jpg

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