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组氨酸-三唑和色氨酸-芘交换对 WHW 肽的影响:Cu(II)结合、DNA/RNA 相互作用和生物活性。

Impact of the Histidine-Triazole and Tryptophan-Pyrene Exchange in the WHW Peptide: Cu(II) Binding, DNA/RNA Interactions and Bioactivity.

机构信息

Division of Organic Chemistry and Biochemistry, Ruđer Bošković Institute, Bijenička Cesta 54, 10000 Zagreb, Croatia.

Division of Molecular Biology, Ruđer Bošković Institute, Bijenička Cesta 54, 10000 Zagreb, Croatia.

出版信息

Int J Mol Sci. 2022 Jun 23;23(13):7006. doi: 10.3390/ijms23137006.

Abstract

In three novel peptidoids based on the tryptophan-histidine-tryptophan (WHW) peptide, the central histidine was replaced by Ala-(triazole), and two derivatives also had one tryptophan replaced with pyrene-alkyls of different lengths and flexibility. Pyrene analogues show strong fluorescence at 480-500 nm, attributed to intramolecular exciplex formation with tryptophan. All three peptidoids bind Cu cation in water with strong affinity, with Trp- Ala-(triazole)-Trp binding comparably to the parent WHW, and the pyrene analogues even stronger, demonstrating that replacement of histidine with triazole in peptides does not hamper Cu coordination. The studied peptidoids strongly bind to ds-DNA and ds-RNA, whereby their complexes with Cu exhibit distinctively different interactions in comparison to metal-free analogues, particularly in the stabilization of ds-DNA against thermal denaturation. The pyrene peptidoids efficiently enter living cells with no apparent cytotoxic effect, whereby their red-shifted emission compared to the parent pyrene allows intracellular confocal microscopy imaging, showing accumulation in cytoplasmic organelles. However, irradiation with 350 nm light resulted in evident antiproliferative effect on cells treated with micromolar concentrations of the pyrene analogues, presumably attributed to pyrene-induced production of singlet oxygen and consecutive cellular damage.

摘要

在三种基于色氨酸-组氨酸-色氨酸 (WHW) 肽的新型肽中,中心组氨酸被丙氨酸-(三唑)取代,两种衍生物还将一个色氨酸替换为不同长度和柔韧性的芘基烷基。芘类似物在 480-500nm 处显示出强荧光,归因于与色氨酸形成分子内激基复合物。所有三种肽都在水中与 Cu 阳离子强烈结合,Trp-Ala-(三唑)-Trp 的结合与母体 WHW 相当,而芘类似物甚至更强,表明在肽中用三唑取代组氨酸不会阻碍 Cu 配位。研究的肽强烈结合 ds-DNA 和 ds-RNA,其与 Cu 的复合物与无金属类似物相比表现出明显不同的相互作用,特别是在稳定 ds-DNA 免受热变性方面。芘肽能够进入活细胞而没有明显的细胞毒性作用,与母体芘相比,其红移发射允许进行细胞内共聚焦显微镜成像,显示在细胞质细胞器中的积累。然而,用 350nm 光照射以微摩尔浓度处理的芘类似物的细胞会产生明显的抗增殖作用,这可能归因于芘诱导的单线态氧的产生和随后的细胞损伤。

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