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携带镍(II)螯合剂的精氨酸载体肽以促进组氨酸标签蛋白的细胞摄取。

Arginine carrier peptide bearing Ni(II) chelator to promote cellular uptake of histidine-tagged proteins.

作者信息

Futaki Shiroh, Niwa Miki, Nakase Ikuhiko, Tadokoro Akiko, Zhang Youjun, Nagaoka Makoto, Wakako Naoya, Sugiura Yukio

机构信息

Institute for Chemical Research, Kyoto University, Uji, Kyoto 611-0011, Japan.

出版信息

Bioconjug Chem. 2004 May-Jun;15(3):475-81. doi: 10.1021/bc034181g.

Abstract

Arginine-rich peptide-mediated protein delivery into living cells is a novel technology for controlling cell functions with therapeutic potential. In this report, a novel approach for the intracellular delivery of histidine-tagged proteins was introduced where a Ni(II) chelate of octaarginine peptide bearing nitrilotriacetic acid [R8-NTA-Ni(II)] was used as a membrane-permeable carrier molecule. Significant internalization of histidine-tagged enhanced green fluorescent protein (EGFP) into HeLa cells was observed by confocal microscopic observation in the presence of R8-NTA-Ni(II). Nuclear condensation characteristic in apoptotic cell death was also induced in the cells treated with a histidine-tagged apoptosis-inducing peptide [pro-apoptotic domain peptide (PAD)], indicating that the cargo molecules really went through the membrane to reach the cytosol. The apoptosis-inducing activity of the peptide thus delivered was compared with that of the PAD peptide covalently connected with the octaarginine peptide.

摘要

富含精氨酸的肽介导的蛋白质递送至活细胞是一种具有治疗潜力的控制细胞功能的新技术。在本报告中,引入了一种用于细胞内递送组氨酸标记蛋白的新方法,其中带有次氮基三乙酸的八聚精氨酸肽的镍(II)螯合物[R8-NTA-Ni(II)]用作膜渗透性载体分子。在存在R8-NTA-Ni(II)的情况下,通过共聚焦显微镜观察,观察到组氨酸标记的增强型绿色荧光蛋白(EGFP)大量内化进入HeLa细胞。在用组氨酸标记的凋亡诱导肽[促凋亡结构域肽(PAD)]处理的细胞中也诱导了凋亡细胞死亡中的核浓缩,表明货物分子确实穿过膜到达细胞质。将如此递送的肽的凋亡诱导活性与与八聚精氨酸肽共价连接的PAD肽的凋亡诱导活性进行了比较。

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